CROSS-REFERENCE TO RELATED APPLICATIONS This application claims benefit of and priority to U.S. Ser. No. 61/142,830, filed Jan. 6, 2009, U.S. Ser. No. 61/151,445, filed Feb. 10, 2009, U.S. Ser. No. 61/243,905, filed Sep. 18, 2009, and U.S. Ser. No. 61/243,930, filed Sept. 18, 2009, all of which are incorporated herein by reference in their entirety for all purposes.
STATEMENT OF GOVERNMENTAL SUPPORT [Not Applicable]
FIELD OF THE INVENTION The present invention relates to novel targeting peptides, novel antimicrobial peptides, chimeric moieties comprising novel targeting and/or novel antimicrobial peptides and uses thereof.
BACKGROUND OF THE INVENTION Antibiotic research at the industrial level was originally focused on the identification of refined variants of already existing drugs. This resulted example, in the development of antibiotics such as newer penicillins, cephalosporins, macrolides, and fluoroquinolones.
However, resistance to old and newer antibiotics among bacterial pathogens is evolving rapidly, as exemplified by extended beta-lactamase (ESBL) and quinolone resistant gram-negatives, multi-resistant gonococci, methicillin resistant Staphylococcus aureus (MRSA), vancomycin resistant enterococci (VRE), penicillin non-susceptible pneumococci (PNSP) and macrolide resistant pneumococci and streptococci (see, e.g., Panlilo et al. (1992) Infect Control Hosp Epidemio., 13: 582-586; Morris et al. (1995) Ann Intern Me., d 123: 250-259, and the like). An overuse, or improper use, of antibiotics is believed to be of great importance for triggering and spread of drug resistant bacteria. Microbes have, in many cases, adapted and are resistant to antibiotics due to constant exposure and improper use of the drugs.
Drug resistant pathogens represent a major economic burden for health-care systems. For example, postoperative and other nosocomial infections will prolong the need for hospital care and increase antibiotic drug expenses. It is estimated that the annual cost of treating drug resistant infections in the United States is approximately $5 billion.
SUMMARY OF THE INVENTION In certain embodiments, novel targeting moieties (e.g., peptides) that specifically/preferentially bind to microorganisms (e.g., certain bacteria, yeasts, fungi, molds, viruses, algae, protozoa, and the like) are provided. The targeting moieties can be attached to effectors (e.g., detectable labels, drugs, antimicrobial peptides, etc.) to form chimeric constructs for specifically/preferentially delivering the effector to and/or into the target organism. In certain embodiments novel antimicrobial peptides that can be used to inhibit (e.g., kill and/or inhibit growth and/or proliferation) of certain microorganisms (e.g., certain bacteria, yeasts, fungi, molds, viruses, algae, protozoa, and the like) are provided.
Accordingly, in certain embodiments, a chimeric construct (chimeric moiety) is provided comprising: an effector attached to a peptide targeting moiety comprising an amino acid sequence found in Table 3 and/or Table 12; and/or an antimicrobial peptide comprising an amino acid sequence found in Table 4 and/or Table 5 attached to a targeting moiety. In certain embodiments the targeting moiety is a peptide comprising an amino acid sequence of a peptide found one or more of Table 3 and Table 12. In certain embodiments the targeting moiety is a peptide comprising two or more amino acid sequences of a peptide found one or more of Table 3 and Table 12. In certain embodiments the targeting moiety is a peptide whose amino acid sequence consists of the amino acid sequence of a peptide found in Table 3.
In various embodiments the effector comprises a moiety selected from the group consisting of an antimicrobial peptide, an antibiotic, a ligand, a lipid or liposome, a agent that physically disrupts the extracellular matrix within a community of microorganisms, and a polymeric particle. In certain embodiments the effector comprises an antimicrobial peptide comprising an amino acid sequence found in one or more of Tables 4, 5, 14, and Table 15. In certain embodiments the effector comprises an antimicrobial peptide comprising an amino acid sequence found in one or more of Tables 4, and 5. In certain embodiments the effector comprises an antimicrobial peptide comprising an amino acid sequence characterized by a motif selected from the group consisting of KIF, FIK, KIH, HIK, and KIV (e.g., as identified in Table 7). In certain embodiments the construct comprises a targeting peptide comprising an amino acid sequence found in Table 3 attached to an antimicrobial peptide comprising an amino acid sequence found in Table 4 and/or Table 5. In certain embodiments the construct comprises an antimicrobial peptide comprising an amino acid sequence found in Table 4 attached to a targeting moiety comprising an amino acid sequence found in Table 3 and/or Table 10, and/or Table 12. In certain embodiments the construct comprises a targeting peptide comprising an amino acid sequence found in Table 3 attached to an antimicrobial peptide comprising an amino acid sequence found in Table 4.
In various embodiments the targeting moiety is chemically conjugated to the effector (directly or via a linker). In certain embodiments the liker comprises a polyethylene glycol (PEG). In certain embodiments the targeting moiety is chemically conjugated to the effector via a non-peptide linker found in Table 16. In certain embodiments the targeting moiety is linked to the effector via a peptide linkage. In certain embodiments the effector comprises an antimicrobial peptide and the construct is a fusion protein. In certain embodiments the targeting moiety is attached to the effector by a peptide linker comprising or consisting of an amino acid sequence found in Table 16. In certain embodiments any of the constructs and/or peptides described herein bears one or more protecting groups. In certain embodiments the one or more protecting groups are independently selected from the group consisting of acetyl, amide, 3 to 20 carbon alkyl groups, fmoc, tboc, 9-fluoreneacetyl group, 1-fluorenecarboxylic group, 9-florenecarboxylic group, 9-fluorenone-1-carboxylic group, benzyloxycarbonyl, xanthyl (Xan), trityl (Trt), 4-methyltrityl (Mtt), 4-methoxytrityl (Mmt), 4-methoxy-2,3,6-trimethyl-benzenesulphonyl (Mtr), mesitylene-2-sulphonyl (Mts), 4,4-dimethoxybenzhydryl (Mbh), tosyl (Tos), 2,2,5,7,8-pentamethyl chroman-6-sulphonyl (Pmc), 4-methylbenzyl (MeBzl), 4-methoxybenzyl (MeOBzl), benzyloxy (BzlO), benzyl (Bzl), benzoyl (Bz), 3-nitro-2-pyridinesulphenyl (Npys), 1-(4,4-dimentyl-2,6-diaxocyclohexylidene)ethyl (Dde), 2,6-dichlorobenzyl (2,6-DiCl-Bzl), 2-chlorobenzyloxycarbonyl (2-Cl-Z), 2-bromobenzyloxycarbonyl (2-Br-Z), benzyloxymethyl (Bom), t-butoxycarbonyl (Boc), cyclohexyloxy (cHxO), t-butoxymethyl (Bum), t-butoxy (tBuO), t-Butyl (tBu), and trifluoroacetyl (TFA). In certain embodiments the peptide and/or construct comprises a protecting group at a carboxyl and/or amino terminus. In certain embodiments the carboxyl terminus is amidated and/or the amino terminus is acetylated. In various embodiments the chimeric construct and/or peptide is functionalized with a polymer (e.g., comprises polyethylene glycol, cellulose, modified cellulose, dextrin, etc.) to increase serum halflife.
In certain embodiments pharmaceutical compositions are provided. In various embodiments the pharmaceutical compositions comprise a chimeric construct as described herein (e.g., a chimeric construct according to any of claims 1-26) and/or an antimicrobial peptide as described herein, in a pharmaceutically acceptable carrier. In certain embodiments the composition is formulated as a unit dosage formulation. In certain embodiments the composition is formulated for administration by a modality selected from the group consisting of intraperitoneal administration, topical administration, oral administration, inhalation administration, transdermal administration, subdermal depot administration, systemic IV application, ocular administration, and rectal administration.
In certain embodiments isolated antimicrobial peptides are provided. In various embodiments the peptides comprise one or more sequences selected from the amino acid sequences listed in Table 4 and/or Table 5 (and/or the retro, inverso, retroinverso, or beta forms). In various embodiments the antimicrobial peptide bears one or more protecting groups e.g., as described herein.
In certain embodiments a composition effective to kill or to inhibit the growth and/or of a microorganism and/or the formation and/or maintenance of a biofilm is provided. The composition typically comprises one or more isolated antimicrobial peptides, the amino acid sequences of the peptides comprising one or more sequences selected from the amino acid sequences listed in Table 4 and/or Table 5 (and/or their retro, inverso, or retroinverso forms). In certain embodiments the composition is effective to kill or inhibit the growth and/or proliferation of a yeast or fungus, and the composition comprises one or more peptides, the amino acid sequences of the peptides comprising one or more sequences selected from the group of amino acid sequences listed in Table 4 and/or Table 5 identified (e.g., in those tables) as effective to effective to kill or inhibit the growth and/or proliferation of a yeast or fungus. In certain embodiments the composition is effective to kill or inhibit the growth and/or proliferation of Aspergillus niger and the composition comprises one or more peptides, the amino acid sequences of the peptides comprising one or more sequences selected from the group of amino acid sequences listed in Table 4 and/or Table 5 identified as effective to effective to kill or inhibit the growth and/or proliferation of Aspergillus niger. In certain embodiments the composition is effective to kill or inhibit the growth and/or proliferation of C. albicans and the composition comprises one or more peptides, the amino acid sequences of the peptides comprising one or more sequences selected from the group of amino acid sequences listed in Table 4 and/or Table 5 identified as effective to effective to kill or inhibit the growth and/or proliferation of C. albicans. In certain embodiments the composition is effective to kill or inhibit the growth and/or proliferation of T. rubrum and the composition comprises one or more peptides, the amino acid sequences of the peptides comprising one or more sequences selected from the group of amino acid sequences listed in Table 4 and/or Table 5 identified as effective to effective to kill or inhibit the growth and/or proliferation of T. rubrum. In certain embodiments the composition is effective to kill or inhibit the growth and/or proliferation of a bacterium, and the composition comprises one or more peptides, the amino acid sequences of the peptides comprising one or more sequences selected from the group of amino acid sequences listed in Table 4 and/or Table 5 identified as effective to effective to kill or inhibit the growth and/or proliferation of a bacterium. In certain embodiments the composition is effective to kill or inhibit the growth and/or proliferation of a gram positive bacterium, and the composition comprises one or more peptides, the amino acid sequences of the peptides comprising one or more sequences selected from the group of amino acid sequences listed in Table 4 and/or Table 5 identified as effective to effective to kill or inhibit the growth and/or proliferation of a gram positive bacterium. In certain embodiments the composition is effective to kill or inhibit the growth and/or proliferation of A. naeslundii, and the composition comprises one or more peptides, the amino acid sequences of the peptides comprising one or more sequences selected from the group of amino acid sequences listed in Table 4 and/or Table 5 identified as effective to effective to kill or inhibit the growth and/or proliferation of A. naeslundii. In certain embodiments the composition is effective to kill or inhibit the growth and/or proliferation of B. subtilis, and the composition comprises one or more peptides, the amino acid sequences of the peptides comprising one or more sequences selected from the group of amino acid sequences listed in Table 4 and/or Table 5 identified as effective to effective to kill or inhibit the growth and/or proliferation of B. subtilis. In certain embodiments the composition is effective to kill or inhibit the growth and/or proliferation of C. difficile, and the composition comprises one or more peptides, the amino acid sequences of the peptides comprising one or more sequences selected from the group of amino acid sequences listed in Table 4 and/or Table 5 identified as effective to effective to kill or inhibit the growth and/or proliferation of C. difficile. In certain embodiments the composition is effective to kill or inhibit the growth and/or proliferation of C. jeikeium, and the composition comprises one or more peptides, the amino acid sequences of the peptides comprising one or more sequences selected from the group of amino acid sequences listed in Table 4 and/or Table 5 identified as effective to effective to kill or inhibit the growth and/or proliferation of C. jeikeium. In certain embodiments the composition is effective to kill or inhibit the growth and/or proliferation of E. faecalis, and the composition comprises one or more peptides, the amino acid sequences of the peptides comprising one or more sequences selected from the group of amino acid sequences listed in Table 4 and/or Table 5 identified as effective to effective to kill or inhibit the growth and/or proliferation of E. faecalis. In certain embodiments the composition is effective to kill or inhibit the growth and/or proliferation of M. luteus, and the composition comprises one or more peptides, the amino acid sequences of the peptides comprising one or more sequences selected from the group of amino acid sequences listed in Table 4 and/or Table 5 identified as effective to effective to kill or inhibit the growth and/or proliferation of M. luteus. In certain embodiments the composition is effective to kill or inhibit the growth and/or proliferation of MRSA, and the composition comprises one or more peptides, the amino acid sequences of the peptides comprising one or more sequences selected from the group of amino acid sequences listed in Table 4 and/or Table 5 identified as effective to effective to kill or inhibit the growth and/or proliferation of MRSA. In certain embodiments composition is effective to kill or inhibit the growth and/or proliferation of S. epidermidis, and the composition comprises one or more peptides, the amino acid sequences of the peptides comprising one or more sequences selected from the group of amino acid sequences listed in Table 4 and/or Table 5 identified as effective to effective to kill or inhibit the growth and/or proliferation of S. epidermidis. In certain embodiments the composition is effective to kill or inhibit the growth and/or proliferation of S. mutans, and the composition comprises one or more peptides, the amino acid sequences of the peptides comprising one or more sequences selected from the group of amino acid sequences listed in Table 4 and/or Table 5 identified as effective to effective to kill or inhibit the growth and/or proliferation of S. mutans. In certain embodiments the composition is effective to kill or inhibit the growth and/or proliferation of S. pneumoniae, and the composition comprises one or more peptides, the amino acid sequences of the peptides comprising one or more sequences selected from the group of amino acid sequences listed in Table 4 and/or Table 5 identified as effective to effective to kill or inhibit the growth and/or proliferation of S. pneumoniae. In certain embodiments the composition is effective to kill or inhibit the growth and/or proliferation of a gram negative bacterium, and the composition comprises one or more peptides, the amino acid sequences of the peptides comprising one or more sequences selected from the group of amino acid sequences listed in Table 4 and/or Table 5 identified as effective to effective to kill or inhibit the growth and/or proliferation of a gram negative bacterium. In certain embodiments the composition is effective to kill or inhibit the growth and/or proliferation of A. baumannii, and the composition comprises one or more peptides, the amino acid sequences of the peptides comprising one or more sequences selected from the group of amino acid sequences listed in Table 4 and/or Table 5 identified as effective to effective to kill or inhibit the growth and/or proliferation of A. baumannii. In certain embodiments the composition is effective to kill or inhibit the growth and/or proliferation of C. jejuni, and the composition comprises one or more peptides, the amino acid sequences of the peptides comprising one or more sequences selected from the group of amino acid sequences listed in Table 4 and/or Table 5 identified as effective to effective to kill or inhibit the growth and/or proliferation of C. jejuni. In certain embodiments the composition is effective to kill or inhibit the growth and/or proliferation of E. coli, and the composition comprises one or more peptides, the amino acid sequences of the peptides comprising one or more sequences selected from the group of amino acid sequences listed in Table 4 and/or Table 5 identified as effective to effective to kill or inhibit the growth and/or proliferation of E. coli. In certain embodiments the composition is effective to kill or inhibit the growth and/or proliferation of F. nucleatum, and the composition comprises one or more peptides, the amino acid sequences of the peptides comprising one or more sequences selected from the group of amino acid sequences listed in Table 4 and/or Table 5 identified as effective to effective to kill or inhibit the growth and/or proliferation of F. nucleatum. In certain embodiments the composition is effective to kill or inhibit the growth and/or proliferation of E. coli, and the composition comprises one or more peptides, the amino acid sequences of the peptides comprising one or more sequences selected from the group of amino acid sequences listed in Table 4 and/or Table 5 identified as effective to effective to kill or inhibit the growth and/or proliferation of M. xanthus. In certain embodiments the composition is effective to kill or inhibit the growth and/or proliferation of P. aeruginosa, and the composition comprises one or more peptides, the amino acid sequences of the peptides comprising one or more sequences selected from the group of amino acid sequences listed in Table 4 and/or Table 5 identified as effective to effective to kill or inhibit the growth and/or proliferation of P. aeruginosa. In certain embodiments the composition is effective to kill or inhibit the growth and/or proliferation of P. gingivalis, and the composition comprises one or more peptides, the amino acid sequences of the peptides comprising one or more sequences selected from the group of amino acid sequences listed in Table 4 and/or Table 5 identified as effective to effective to kill or inhibit the growth and/or proliferation of P. gingivalis. In certain embodiments the composition is effective to kill or inhibit the growth and/or proliferation of P. mirabilis, and the composition comprises one or more peptides, the amino acid sequences of the peptides comprising one or more sequences selected from the group of amino acid sequences listed in Table 4 and/or Table 5 identified as effective to effective to kill or inhibit the growth and/or proliferation of P. mirabilis.
In various embodiments one or more of the peptides comprising the composition comprise all “L” amino acids or all “D” amino acids, or a mixture of “L” and “D” amino acids. In various embodiments one or more of the peptides comprising the composition are β peptides. In various embodiments one or more of the peptides comprising the composition comprise one or more protecting groups (e.g. protected carboxyl and/or amino termini). In various embodiments one or more of the peptides comprising the composition comprise an amide on the carboxyl terminus and/or an acetyl on the amino terminus. In various embodiments the peptides comprising the composition are in a pharmaceutically acceptable carrier. In certain embodiments the carrier is suitable for administration via a route selected from the group consisting of topical administration, aerosol administration, administration via inhalation, oral administration, and/or rectal administration.
In various embodiments methods are provided for killing and/or inhibiting the growth and/or proliferation of a microorganism and or for disrupting and/or inhibiting the growth and/or maintenance of a biofilm, the method comprising contacting the microorganism (or a biofilm comprising the microorganism) with a chimeric construct as described herein (e.g., see description above, and/or a chimeric construct according to any one of claims 1-29), or with an antimicrobial peptide as described herein, and/or with a composition as described herein (e.g., a composition according to any one of claims 30-65). In certain embodiments the microorganism is a yeast or fungus and the chimeric construct or composition is a chimeric construct comprising an effector identified as killing a yeast or fungus, or a composition comprising an antimicrobial peptide described herein as killing a yeast or fungus. In certain embodiments the microorganism is a bacterium (e.g., gram negative and/or gram positive bacterium) and the chimeric construct or composition is a chimeric construct comprising an effector identified as killing a bacterium (e.g., gram negative and/or gram positive bacterium), or a composition comprising an antimicrobial peptide described herein as killing a gram negative and/or gram positive bacterium. In certain embodiments the effector is an antimicrobial peptide. In certain embodiments he microorganism is S. mutans, and the chimeric construct or composition is applied to the oral cavity of an animal or human, e.g., to reduces the incidence or severity of dental caries and/or periodontal disease). In certain embodiments the chimeric construct or composition preferentially targets Corynebacterium spp. and the chimeric construct or composition is applied to the skin surface of an animal or human (e.g., to reduce body odor).
Methods are also provided for disinfecting a surface. The methods typically involve contacting the surface with one or more chimeric constructs described herein (e.g. a construct according to any one of claims 1-29), or a composition as described herein (e.g., a composition according to any one of claims 30-65). In certain embodiments, the surface comprises a surface of a prosthesis or medical implant. In certain embodiments the surface comprises a surface of a medical device. In certain embodiments the surface comprises a surface of a plant or foodstuff. In certain embodiments the chimeric construct and/or the antimicrobial peptide(s) are combined with a second disinfectant selected from the group consisting of other antimicrobial agent is a disinfectant selected from the group consisting of acetic acid, phosphoric acid, citric acid, lactic, formic, propionic acid, hydrochloric acid, sulfuric acid, nitric acid, sodium hydroxide, potassium hydroxide, sodium carbonate, ammonium hydroxide, ethyl alcohol, isopropyl alcohol, phenol, formaldehyde, glutaraldehyde, hypochlorites, chlorine dioxide, sodium dichloroisocyanurate, chloramine-T, iodine, povidone-iodine, chlorhexidine, hydrogen peroxide, peracetic acid, and benzalkonium chloride.
In various embodiments the use of a chimeric construct described herein and/or an antimicrobial composition as described herein (e.g., a chimeric construct according to any one of claims 1-29, or a composition according to any one of claims 30-65) in the manufacture of a medicament for killing and/or inhibiting the growth and/or proliferation of a microorganism and/or inhibiting the growth and/or maintenance of a biofilm comprising the microorganism is provided. In certain embodiments the microorganism is a yeast or fungus and the chimeric construct or composition is a chimeric construct comprising an effector identified as killing a yeast or fungus, or a composition comprising an antimicrobial peptide described herein as killing a yeast or fungus. In certain embodiments the microorganism is a bacterium (e.g., gram negative and/or gram positive bacterium) and the chimeric construct or composition is a chimeric construct comprising an effector identified as killing a bacterium (e.g., gram negative and/or gram positive bacterium), or a composition comprising an antimicrobial peptide described herein as killing a gram negative and/or gram positive bacterium. In certain embodiments the effector is an antimicrobial peptide.
In various embodiments methods are also provided for of detecting a bacterium and/or a bacterial film (e.g., a biofilm comprising the bacteria). The methods typically involve contacting the bacterium or bacterial film with a composition comprising a detectable label attached to a targeting peptide comprising one or more amino acid sequences found Table 3 and/or Table 12; and detecting the detectable label where the quantity and/or location of the detectable label is an indicator of the presence of the bacterium and/or bacterial film. In certain embodiments the targeting peptide comprises or consists of an amino acid sequence of a peptide found in Table 3 (and/or the retro, inverso, retroinverso form of the sequence). In certain embodiments the detectable label is a label selected from the group consisting of a radioactive label, a radio-opaque label, a fluorescent dye, a fluorescent protein, an enzymatic label, a colorimetric label, and a quantum dot.
Certain compositions are also provided comprising a photosensitizing or photoactivatable agent attached to a targeting peptide (e.g., a peptide comprising an amino acid sequence of a peptide found in Table 3 and/or Table 12). In certain embodiments the targeting peptide comprises or consists of an amino acid sequence of a peptide found in Table 3. In certain embodiments the photosensitizing agent is an agent selected from the group consisting of a porphyrinic macrocycle, a porphyrin, a chlorine, a crown ether, an acridine, an azine, a phthalocyanine, a cyanine, a psoralen, a cucumin, and a perylenequinonoid. In certain embodiments the photosensitizing agent comprises one or more agents agent shown in any of FIGS. 1-12. In certain embodiments the photosensitizing agent is attached to the targeting peptide by a non-peptide linker (e.g., a polyethylene glycol (PEG)). In certain embodiments the photosensitizing agent is attached to the targeting peptide by a non-peptide linker found in Table 16.
In various embodiments methods are provided for killing and/or for inhibiting the growth and/or proliferation of a microorganism or a biofilm comprising a microorganism, where the methods involve contacting the microorganism or biofilm with a composition comprising a photosensitizing or photoactivatable agent attached to a targeting peptide (e.g., a peptide comprising an amino acid sequence of a peptide found in Table 3 and/or Table 12). In certain embodiments the targeting peptide comprises or consists of an amino acid sequence of a peptide found in Table 3. In certain embodiments the photosensitizing agent is an agent selected from the group consisting of a porphyrinic macrocycle, a porphyrin, a chlorine, a crown ether, an acridine, an azine, a phthalocyanine, a cyanine, a psoralen, a cucumin, and a perylenequinonoid. In certain embodiments the photosensitizing agent comprises one or more agents agent shown in any of FIGS. 1-12. In certain embodiments the photosensitizing agent is attached to the targeting peptide by a non-peptide linker (e.g., a polyethylene glycol (PEG)). In certain embodiments the photosensitizing agent is attached to the targeting peptide by a non-peptide linker found in Table 16. In certain embodiments the method further comprises exposing the microorganism or biofilm to a light source. In certain embodiments the microorganism is a microorganism selected from the group consisting of a bacterium (e.g., a gram positive and/or a gram negative bacterium), a yeast, a fungus, a protozoan, and a virus. In certain embodiments the biofilm comprises a bacterial film. In certain embodiments the biofilm is a biofilm on an implanted or implantable medical device. In certain embodiments the microorganism or biofilm is an organism or biofilm in an oral cavity.
In various embodiments certain formulations are provided. Typical formulations include, but are not limited to a targeting peptide, an antimicrobial peptide, and/or a STAMP; and a salt at a concentration comparable to that found in phosphate buffered saline (PBS) ranging from about 0.5× PBS to about 2.5× PBS. In certain embodiments the formulation comprises a targeting peptide found in Tables 3 or 10. In certain embodiments the formulation comprises an anti-S. mutans peptide targeting peptide (e.g., as identified in Tables 3 or 12). In certain embodiments the anti-S. mutans targeting peptide has the amino acid sequence TFFRLFNRSFTQALGK (SEQ ID NO:1). In certain embodiments the anti-S. mutans targeting peptide is attached to an antimicrobial peptide. In certain embodiments the antimicrobial peptide is a peptide found in Tables 4, 5, or 14. In certain embodiments the antimicrobial peptide has the amino acid sequence KNLRIIRKGIHIIKKY (SEQ ID NO:3080). In certain embodiments the formulation comprises the amino acid sequence of the C16G2 STAMP (TFFRLFNRSFTQALGKGGGKNLRIIRKGIHIIKKY, (SEQ ID NO:2). In various embodiments the targeting peptide, antimicrobial peptide, and/or a STAMP bears one or more protecting groups. In certain embodiments the protecting group(s) are independently selected from the group consisting of acetyl, amide, 3 to 20 carbon alkyl groups, Fmoc, Tboc, 9-fluoreneacetyl group, 1-fluorenecarboxylic group, 9-florenecarboxylic group, 9-fluorenone-1-carboxylic group, benzyloxycarbonyl, Xanthyl (Xan), Trityl (Trt), 4-methyltrityl (Mtt), 4-methoxytrityl (Mmt), 4-methoxy-2,3,6-trimethyl-benzenesulphonyl (Mtr), Mesitylene-2-sulphonyl (Mts), 4,4-dimethoxybenzhydryl (Mbh), Tosyl (Tos), 2,2,5,7,8-pentamethyl chroman-6-sulphonyl (Pmc), 4-methylbenzyl (MeBzl), 4-methoxybenzyl (MeOBzl), Benzyloxy (BzlO), Benzyl (Bzl), Benzoyl (Bz), 3-nitro-2-pyridinesulphenyl (Npys), 1-(4,4-dimentyl-2,6-diaxocyclohexylidene)ethyl (Dde), 2,6-dichlorobenzyl (2,6-DiCl-Bzl), 2-chlorobenzyloxycarbonyl (2-Cl-Z), 2-bromobenzyloxycarbonyl (2-Br-Z), Benzyloxymethyl (Bom), t-butoxycarbonyl (Boc), cyclohexyloxy (cHxO), t-butoxymethyl (Bum), t-butoxy (tBuO), t-Butyl (tBu), and Trifluoroacetyl (TFA). In certain embodiments the targeting peptide, antimicrobial peptide, and/or a STAMP is amidated at the carboxyl terminus and/or bears an acetyl group at the amino terminus. In certain embodiments the pH of the formulation ranges from about pH 5.0 to about pH 8.5. In certain embodiments the pH is about pH 7.4. In various embodiments the salt is at a concentration comparable to that found in 1× PBS. In certain embodiments the formulation comprises PBS. In certain embodiments the formulation of further comprising ethanol, and/or glycerin, and/or polyethylene glycol, and/or fluoride.
DEFINITIONS The term “peptide” as used herein refers to a polymer of amino acid residues typically ranging in length from 2 to about 50 or about 60 residues. In certain embodiments the peptide ranges in length from about 2, 3, 4, 5, 7, 9, 10, or 11 residues to about 60, 50, 45, 40, 45, 30, 25, 20, or 15 residues. In certain embodiments the peptide ranges in length from about 8, 9, 10, 11, or 12 residues to about 15, 20 or 25 residues. In certain embodiments the amino acid residues comprising the peptide are “L-form” amino acid residues, however, it is recognized that in various embodiments, “D” amino acids can be incorporated into the peptide. Peptides also include amino acid polymers in which one or more amino acid residues is an artificial chemical analogue of a corresponding naturally occurring amino acid, as well as to naturally occurring amino acid polymers. In addition, the term applies to amino acids joined by a peptide linkage or by other, “modified linkages” (e.g., where the peptide bond is replaced by an α-ester, a β-ester, a thioamide, phosphonamide, carbonate, hydroxylate, and the like (see, e.g., Spatola, (1983) Chem. Biochem. Amino Acids and Proteins 7: 267-357), where the amide is replaced with a saturated amine (see, e.g., Skiles et al., U.S. Pat. No. 4,496,542, which is incorporated herein by reference, and Kaltenbronn et al., (1990) Pp. 969-970 in Proc. 11th American Peptide Symposium, ESCOM Science Publishers, The Netherlands, and the like)).
The term “residue”” as used herein refers to natural, synthetic, or modified amino acids. Various amino acid analogues include, but are not limited to 2-aminoadipic acid, 3-aminoadipic acid, beta-alanine (beta-aminopropionic acid), 2-aminobutyric acid, 4-aminobutyric acid, piperidinic acid, 6-aminocaproic acid, 2-aminoheptanoic acid, 2-aminoisobutyric acid, 3-aminoisobutyric acid, 2-aminopimelic acid, 2,4 diaminobutyric acid, desmosine, 2,2′-diaminopimelic acid, 2,3-diaminopropionic acid, n-ethylglycine, n-ethylasparagine, hydroxylysine, allo-hydroxylysine, 3-hydroxyproline, 4-hydroxyproline, isodesmosine, allo-isoleucine, n-methylglycine, sarcosine, n-methylisoleucine, 6-n-methyllysine, n-methylvaline, norvaline, norleucine, ornithine, and the like. These modified amino acids are illustrative and not intended to be limiting.
“β-peptides” comprise of “β amino acids”, which have their amino group bonded to the β carbon rather than the α-carbon as in the 20 standard biological amino acids. The only commonly naturally occurring β amino acid is β-alanine
Peptoids, or N-substituted glycines, are a specific subclass of peptidomimetics. They are closely related to their natural peptide counterparts, but differ chemically in that their side chains are appended to nitrogen atoms along the molecule's backbone, rather than to the α-carbons (as they are in natural amino acids).
The terms “conventional” and “natural” as applied to peptides herein refer to peptides, constructed only from the naturally-occurring amino acids: Ala, Cys, Asp, Glu, Glu, Phe, Gly, His, Ile, Lys, Leu, Met, Asn, Pro, Gln, Arg, Ser, Thr, Val, Trp, and Tyr. A compound of the invention “corresponds” to a natural peptide if it elicits a biological activity (e.g., antimicrobial activity) related to the biological activity and/or specificity of the naturally occurring peptide. The elicited activity may be the same as, greater than or less than that of the natural peptide. In general, such a peptoid will have an essentially corresponding monomer sequence, where a natural amino acid is replaced by an N-substituted glycine derivative, if the N-substituted glycine derivative resembles the original amino acid in hydrophilicity, hydrophobicity, polarity, etc. The following are illustrative, but non-limiting N-substituted glycine replacements: N-(1-methylprop-1-yl)glycine substituted for isoleucine (Ile), N-(prop-2-yl)glycine for valine (Val), N-benzylglycine for phenylanlaine (Phe), N-(2-hydroxyethyl)glycine for serine (Ser), and the like. In certain embodiments substitutions need not be “exact”. Thus for example, in certain embodiments N-(2-hydroxyethyl)glycine may substitute for Ser, Thr, Cys, and/or Met; N-(2-methylprop-1-yl)glycine may substitute for Val, Leu, and/or Ile. In certain embodiments N-(2-hydroxyethyl)glycine can be used to substitute for Thr and Ser, despite the structural differences: the side chain in N-(2-hydroxyethyl)glycine is one methylene group longer than that of Ser, and differs from Thr in the site of hydroxy-substitution. In general, one may use an N-hydroxyalkyl-substituted glycine to substitute for any polar amino acid, an N-benzyl-or N-aralkyl-substituted glycine to replace any aromatic amino acid (e.g., Phe, Trp, etc.), an N-alkyl-substituted glycine such as N-butylglycine to replace any nonpolar amino acid (e.g., Leu, Val, Ile, etc.), and an N-(aminoalkyl)glycine derivative to replace any basic polar amino acid (e.g., Lys and Arg).
Where an amino acid sequence is provided herein, L-, D-, or beta amino acid versions of the sequence are also contemplated as well as retro, inversion, and retro-inversion isoforms. In addition, conservative substitutions (e.g., in the binding peptide, and/or antimicrobial peptide, and/or linker peptide) are contemplated. Non-protein backbones, such as PEG, alkane, ethylene bridged, ester backbones, and other backbones are also contemplated. Also fragments ranging in length from about 5, 6, 7, 8, 9, 10, 11, 12, 13, 14, 15, 16, 17, 18, 19, 20, 21, 22, 23, 24, or 25 amino acids up to the full length minus one amino acid of the peptide are contemplated where the fragment retains at least 50%, preferably at least 60% 70% or 80%, more preferably at least 90%, 95%, 98%, 99%, or at least 100% of the activity (e.g., binding specificity and/or avidity, antimicrobial activity, etc.) of the full length peptide are contemplated.
A “compound antimicrobial peptide” or “compound AMP” refers to a construct comprising two or more AMPs joined together. The AMPs can be joined directly or through a linker. They can be chemically conjugated or, where joined directly together or through a peptide linker can comprise a fusion protein.
In certain embodiments, conservative substitutions of the amino acids comprising any of the sequences described herein are contemplated. In various embodiments one, two, three, four, or five different residues are substituted. The term “conservative substitution” is used to reflect amino acid substitutions that do not substantially alter the activity (e.g., antimicrobial activity and/or specificity) of the molecule. Typically conservative amino acid substitutions involve substitution one amino acid for another amino acid with similar chemical properties (e.g. charge or hydrophobicity). Certain conservative substitutions include “analog substitutions” where a standard amino acid is replaced by a non-standard (e.g., rare, synthetic, etc) amino acid differing minimally from the parental residue. Amino acid analogs are considered to be derived synthetically from the standard amino acids without sufficient change to the structure of the parent, are isomers, or are metabolite precursors. Examples of such “analog substitutions” include, but are not limited to, 1) Lys-Orn, 2) Leu-Norleucine, 3) Lys-Lys[TFA], 4) Phe-Phe[Gly], and 5) δ-amino butylglycine-ξ-amino hexylglycine, where Phe[gly] refers to phenylglycine(a Phe derivative with a H rather than CH3 component in the R group), and Lys[TFA] refers to a Lys where a negatively charged ion (e.g., TFA) is attached to the amine R group. Other conservative substitutions include “functional substitutions” where the general chemistries of the two residues are similar, and can be sufficient to mimic or partially recover the function of the native peptide. Strong functional substitutions include, but are not limited to 1) Gly/Ala, 2) Arg/Lys, 3) Ser/Tyr/Thr, 4) Leu/Ile/Val, 5) Asp/Glu, 6) Gln/Asn, and 7) Phe/Trp/Tyr, while other functional substitutions include, but are not limited to 8) Gly/Ala/Pro, 9) Tyr/His, 10) Arg/Lys/His, 11) Ser/Thr/Cys, 12) Leu/Ile/Val/Met, and 13) Met/Lys (special case under hydrophobic conditions). Various “broad conservative substations” include substitutions where amino acids replace other amino acids from the same biochemical or biophysical grouping. This is similarity at a basic level and stems from efforts to classify the original 20 natural amino acids. Such substitutions include 1) nonpolar side chains: Gly/Ala/Val/Leu/Ile/Met/Pro/Phe/Trp, and/or 2) uncharged polar side chains Ser/Thr/Asn/Gln/Tyr/Cys. In certain embodiments broad-level substitutions can also occur as paired substitutions. For example, Any hydrophilic neutral pair [Ser, Thr, Gln, Asn, Tyr, Cys]+[Ser, Thr, Gln, Asn, Tyr, Cys] can may be replaced by a charge-neutral charged pair [Arg, Lys, His]+[Asp, Glu]. The following six groups each contain amino acids that, in certain embodiments, are typical conservative substitutions for one another: 1) Alanine (A), Serine (S), Threonine (T); 2) Aspartic acid (D), Glutamic acid (E); 3) Asparagine (N), Glutamine (Q); 4) Arginine (R), Lysine (K), Histidine (H); 5) Isoleucine (I), Leucine (L), Methionine (M), Valine (V); and 6) Phenylalanine (F), Tyrosine (Y), Tryptophan (W). Where amino acid sequences are disclosed herein, amino acid sequences comprising, one or more of the above-identified conservative substitutions are also contemplated.
In certain embodiments, targeting peptides, antimicrobial peptides, and/or STAMPs compromising at least 80%, preferably at least 85% or 90%, and more preferably at least 95% or 98% sequence identity with any of the sequences described herein are also contemplated. The terms “identical” or percent “identity,” refer to two or more sequences that are the same or have a specified percentage of amino acid residues that are the same, when compared and aligned for maximum correspondence, as measured using one of the following sequence comparison algorithms or by visual inspection. With respect to the peptides of this invention sequence identity is determined over the full length of the peptide. For sequence comparison, typically one sequence acts as a reference sequence, to which test sequences are compared. When using a sequence comparison algorithm, test and reference sequences are input into a computer, subsequence coordinates are designated, if necessary, and sequence algorithm program parameters are designated. The sequence comparison algorithm then calculates the percent sequence identity for the test sequence(s) relative to the reference sequence, based on the designated program parameters. Optimal alignment of sequences for comparison can be conducted, e.g., by the local homology algorithm of Smith & Waterman (1981) Adv. Appl. Math. 2: 482, by the homology alignment algorithm of Needleman & Wunsch (1970) J. Mol. Biol. 48: 443, by the search for similarity method of Pearson & Lipman (1988) Proc. Natl. Acad. Sci., USA, 85: 2444, by computerized implementations of these algorithms (GAP, BESTFIT, FASTA, and TFASTA in the Wisconsin Genetics Software Package, Genetics Computer Group, 575 Science Dr., Madison, Wis.), or by visual inspection.
The term “specificity” when used with respect to the antimicrobial activity of a peptide indicates that the peptide preferentially inhibits growth and/or proliferation and/or kills a particular microbial species as compared to other related and/or unrelated microbes. In certain embodiments the preferential inhibition or killing is at least 10% greater (e.g., LD50 is 10% lower), preferably at least 20%, 30%, 40%, or 50%, more preferably at least 2-fold, at least 5-fold, or at least 10-fold greater for the target species.
“Treating” or “treatment” of a condition as used herein may refer to preventing the condition, slowing the onset or rate of development of the condition, reducing the risk of developing the condition, preventing or delaying the development of symptoms associated with the condition, reducing or ending symptoms associated with the condition, generating a complete or partial regression of the condition, or some combination thereof.
The term “consisting essentially of” when used with respect to an antimicrobial peptide (AMP) or AMP motif as described herein, indicates that the peptide or peptides encompassed by the library or variants, analogues, or derivatives thereof possess substantially the same or greater antimicrobial activity and/or specificity as the referenced peptide. In certain embodiments substantially the same or greater antimicrobial activity indicates at least 80%, preferably at least 90%, and more preferably at least 95% of the anti microbial activity of the referenced peptide(s) against a particular bacterial species (e.g., S. mutans).
The term “porphyrinic macrocycle” refers to a porphyrin or porphyrin derivative. Such derivatives include porphyrins with extra rings ortho-fused, or orthoperifused, to the porphyrin nucleus, porphyrins having a replacement of one or more carbon atoms of the porphyrin ring by an atom of another element (skeletal replacement), derivatives having a replacement of a nitrogen atom of the porphyrin ring by an atom of another element (skeletal replacement of nitrogen), derivatives having substituents other than hydrogen located at the peripheral (meso-, .beta.-) or core atoms of the porphyrin, derivatives with saturation of one or more bonds of the porphyrin (hydroporphyrins, e.g., chlorins, bacteriochlorins, isobacteriochlorins, decahydroporphyrins, corphins, pyrrocorphins, etc.), derivatives obtained by coordination of one or more metals to one or more porphyrin atoms (metalloporphyrins), derivatives having one or more atoms, including pyrrolic and pyrromethenyl units, inserted in the porphyrin ring (expanded porphyrins), derivatives having one or more groups removed from the porphyrin ring (contracted porphyrins, e.g., corrin, corrole) and combinations of the foregoing derivatives (e.g. phthalocyanines, porphyrazines, naphthalocyanines, subphthalocyanines, and porphyrin isomers). Certain porphyrinic macrocycles comprise at least one 5-membered ring.
As used herein, an “antibody” refers to a protein consisting of one or more polypeptides substantially encoded by immunoglobulin genes or fragments of immunoglobulin genes. The recognized immunoglobulin genes include the kappa, lambda, alpha, gamma, delta, epsilon and mu constant region genes, as well as myriad immunoglobulin variable region genes. Light chains are classified as either kappa or lambda. Heavy chains are classified as gamma, mu, alpha, delta, or epsilon, which in turn define the immunoglobulin classes, IgG, IgM, IgA, IgD and IgE, respectively.
A typical immunoglobulin (antibody) structural unit is known to comprise a tetramer. Each tetramer is composed of two identical pairs of polypeptide chains, each pair having one “light” (about 25 kD) and one “heavy” chain (about 50-70 kD). The N-terminus of each chain defines a variable region of about 100 to 110 or more amino acids primarily responsible for antigen recognition. The terms variable light chain (VL) and variable heavy chain (VH) refer to these light and heavy chains respectively.
Antibodies exist as intact immunoglobulins or as a number of well characterized fragments produced by digestion with various peptidases. Thus, for example, pepsin digests an antibody below the disulfide linkages in the hinge region to produce F(ab)′2, a dimer of Fab which itself is a light chain joined to VH-CH1 by a disulfide bond. The F(ab)′2 may be reduced under mild conditions to break the disulfide linkage in the hinge region thereby converting the (Fab′)2 dimer into an Fab′ monomer. The Fab′ monomer is essentially an Fab with part of the hinge region (see, Fundamental Immunology, W. E. Paul, ed., Raven Press, N.Y. (1993), for a more detailed description of other antibody fragments). While various antibody fragments are defined in terms of the digestion of an intact antibody, one of skill will appreciate that such Fab′ fragments may be synthesized de novo either chemically or by utilizing recombinant DNA methodology. Thus, the term antibody, as used herein also includes antibody fragments either produced by the modification of whole antibodies or synthesized de novo using recombinant DNA methodologies, including, but are not limited to, Fab′2, IgG, IgM, IgA, scFv, dAb, nanobodies, unibodies, and diabodies.
In certain embodiments antibodies and fragments of the present invention can be bispecific. Bispecific antibodies or fragments can be of several configurations. For example, bispecific antibodies may resemble single antibodies (or antibody fragments) but have two different antigen binding sites (variable regions). In various embodiments bispecific antibodies can be produced by chemical techniques (Kranz et al. (1981) Proc. Natl. Acad. Sci., USA, 78: 5807), by “polydoma” techniques (see, e.g., U.S. Pat. No. 4,474,893), or by recombinant DNA techniques. In certain embodiments bispecific antibodies of the present invention can have binding specificities for at least two different epitopes, at least one of which is an epitope of a microbial organism. The microbial binding antibodies and fragments can also be heteroantibodies. Heteroantibodies are two or more antibodies, or antibody binding fragments (e.g., Fab) linked together, each antibody or fragment having a different specificity.
The term “STAMP” refers to Specifically Targeted Anti-Microbial Peptides. In various embodiments, a STAMP comprises one or more peptide targeting moieties attached to one or more antimicrobial moieties (e.g., antimicrobial peptides (AMPs)). An MH-STAMP is a STAMP bearing two or more targeting domains (i.e., a multi-headed STAMP).
The terms “isolated” “purified” or “biologically pure” refer to material which is substantially or essentially free from components that normally accompany it as found in its native state. In the case of a peptide, an isolated (naturally occurring) peptide is typically substantially free of components with which it is associated in the cell, tissue, or organism. The term isolated also indicates that the peptide is not present in a phage display, yeast display, or other peptide library.
In various embodiments the amino acid abbreviations shown in Table 1 are used herein.
TABLE 1
Amino acid abbreviations.
Abbreviation
Name 3 Letter 1 Letter
Alanine Ala A
βAlanine (NH2—CH2—CH2—COOH) βAla
Arginine Arg R
Asparagine Asn N
Aspartic Acid Asp D
Cysteine Cys C
Glutamic Acid Glu E
Glutamine Gln Q
Glycine Gly G
Histidine His H
Homoserine Hse —
Isoleucine Ile I
Leucine Leu L
Lysine Lys K
Methionine Met M
Methionine sulfoxide Met (O) —
Methionine methylsulfonium Met (S-Me) —
Norleucine Nle —
Phenylalanine Phe F
Proline Pro P
Serine Ser S
Threonine Thr T
Tryptophan Trp W
Tyrosine Tyr Y
Valine Val V
episilon-aminocaproic acid Ahx J
(NH2—(CH2)5—COOH)
4-aminobutanoic acid gAbu
(NH2—(CH2)3—COOH)
tetrahydroisoquinoline-3- O
carboxylic acid
Lys(N(epsilon)-trifluoroacetyl) K[TFA]
α-aminoisobutyric acid Aib B
BRIEF DESCRIPTION OF THE DRAWINGS FIG. 1 shows some illustrative porphyrins (compounds 92-99) suitable for use as targeting moieties and/or antimicrobial effectors.
FIG. 2 shows some illustrative porphyrins (compounds 100-118) suitable for use as targeting moieties and/or antimicrobial effectors.
FIG. 3 shows some illustrative porphyrins (in particular phthalocyanines) (compounds 119-128) suitable for use as targeting moieties and/or antimicrobial effectors.
FIG. 4 illustrates the structures of two phthalocyanines, Monoastral Fast Blue B and Monoastral Fast Blue G suitable for use as targeting moieties and/or antimicrobial effectors.
FIG. 5 illustrates certain azine photosensitizers suitable for use as targeting moieties and/or antimicrobial effectors in the compositions and methods described herein.
FIG. 6 shows illustrative cyanine suitable for use as targeting moieties and/or antimicrobial effectors in the compositions and methods described herein.
FIG. 7 shows illustrative psoralen (angelicin) photosensitizers suitable for use as targeting moieties and/or antimicrobial effectors in the compositions and methods described herein.
FIG. 8 shows illustrative hypericin and the perylenequinonoid pigments suitable for use as targeting moieties and/or antimicrobial effectors in the compositions and methods described herein.
FIG. 9 shows illustrative acridines suitable for use as targeting moieties and/or antimicrobial effectors in the compositions and methods described herein.
FIG. 10 illustrates the structure of the acridine Rose Bengal.
FIG. 11 illustrates various crown ethers suitable for use as targeting moieties and/or antimicrobial effectors in the compositions and methods described herein.
FIG. 12 illustrates the structure of cumin.
FIG. 13 illustrates an example of a targeted light-activated porphyrin we have constructed: C16-P18 comprising a porphyrin coupled to a C16 (SEQ ID NO:3) targeting sequence.
FIG. 14 schematically shows some illustrative configurations for chimeric constructs described herein. A: Shows a single targeting moiety T1 attached to a single effector E1 by a linker/spacer L. B: Shows multiple targeting moieties T1, T2, T3 attached directly to each other and attached by a linker L to a single effector E1. In various embodiments T1, T2, and T3, can be domains in a fusion protein. C: Shows multiple targeting moieties T1 , T2, T3 attached to each other by linkers L and attached by a linker L to a single effector E1 . In various embodiments T1 , T2, and T3, can be domains in a fusion protein. D: Shows a single targeting moiety T1 attached by a linker L to multiple effectors E1 , E2, and E3 joined directly to each other. E: Shows a single targeting moiety T1 attached by a linker L to multiple effectors E1 , E2, and E3 joined to each other by linkers L. F: Shows multiple targeting moieties joined directly to each other and by a linker L to multiple effectors joined to each other by linkers L. G: Shows multiple targeting moieties joined to each other by linkers L and by a linker L to multiple effectors joined to each other by linkers L. In various embodiments T1 , T2, and T3, and/or E1, E2, and E3 can be domains in a fusion protein. H: Illustrates a branched configuration where multiple targeting moieties are linked to a single effector. I: Illustrates a dual branched configuration where multiple targeting moieties are linked to multiple effectors. J: Illustrates a branched configuration where multiple targeting moieties are linked to multiple effectors where the effectors are joined to each other in a linear configuration.
FIG. 15 illustrates various MH-STAMPs used in Example 1. The design, sequence, and observed mass (m/z) for M8(KH)-20 (SEQ ID NOs:4, 5, and 6), BL(KH)-20 (SEQ ID 7, 8, and 9), and M8(BL)-20 (SEQ ID 10, 11, and 12).
FIGS. 16A and 16B show HPLC and MS spectra of M8(KH)-20. The quality of the completed MH-STAMP was analyzed by HPLC (FIG. 16A) and MALDI mass spectroscopy (FIG. 16B). At UV absorbance 215 nm (260 and 280 nm are also plotted), a single major product was detected by HPLC (* retention volume 11.04 mL). After fraction collection, the correct mass (m/z) for single-charged M8(KH)-20, 4884.91 (marked by *), was observed for this peak. Y-axis: 16A, mAU miliabsorbance units; 16B, percent intensity.
FIG. 17A-17E show growth inhibitory activity of MH-STAMPs. Monocultures of S. mutans (FIG. 17A); P. aeruginosa (FIG. 17B); S. epidermidis (FIG. 17C); S. aureus (FIG. 17D); or E. coli (FIG. 17E); were treated with peptides (as indicated in the figure) for 10 min. Agent was then removed and fresh media returned. Culture recovery was measured over time (OD600). Plots represent the average of at least 3 independent experiments with standard deviations.
FIG. 18 illustrates the selective activity of dual-targeted and single-targeted MH-STAMPs in mixed culture. A mixture of P. aeruginosa (Pa), S. mutans (Sm), E. coli (Ec), and S. epidermidis (Se) planktonic cells were mixed with MH-STAMPs (as indicated in the figure) and treated 24 h. After incubation, cfu/mL of remaining constituent species were quantitated after plating to selective media. * indicates under 200 surviving cfu/mL recovered.
FIGS. 19A and 19B illustrate Rose Bengal (FIG. 19A) and synthesis scheme for C16-RB, halides and side-chains omitted for clarity (FIG. 19B).
FIG. 20 shows LC/MS profile C16-RB. Purity and molecular mass of C16-RB was confirmed by LC/MS. A single product was observed at 11.92 min with mass species at 1040.8 and 1560.25 daltons. Expected C16-RB mas: m/z=3118, m2+/z=1559, m3+/z=1039.
FIG. 21 illustrates activity of RB and C16-RB against single-species S. mutans biofilms. * indicates fewer than 100 cfu/mL recovered
FIG. 22 shows S. mutans-specific C16-RB activity. C16-RB, and not RB alone, preferentially eliminated S. mutans, and not other oral streptococci, after blue light illumination.
DETAILED DESCRIPTION In various embodiments, novel “targeting” peptides are identified that specifically or preferentially bind particular microorganisms (e.g., bacteria, yeasts, fungi, etc.). These peptides can be used alone to bind/capture and thereby identify and/or isolate particular target microorganisms, or they can be attached to one or more effectors (e.g., drugs, labels, etc.) and used as targeting moieties thereby providing a chimeric moiety that preferentially or specifically delivers the effector to a target microorganism, a population of target microorganisms, a microbial film, a biofilm, and the like.
In various embodiments novel peptides having antimicrobial activity against certain bacteria, fungi, yeasts, and/or viruses and/or having activity that inhibits the growth or maintenance of biofilms comprising such microorganisms are provided. The AMPs can be used to inhibit the growth and/or proliferation of a microbial species and/or the growth and/formation and/or maintenance of a biofilm comprising the microbial species.
In certain embodiments, the targeting moieties can be attached to antimicrobial peptides to form Specifically Targeted Anti-Microbial Peptides (STAMPs). In certain embodiments attachment of one or more targeting moieties/peptides to one or more antimicrobial peptides can narrow the spectrum of activity of the AMP(s) to provide efficacy against one or a few target microorganisms without substantially disrupting the remaining microbial ecology and thereby provide increased efficacy with fewer side effects.
In certain embodiments STAMPs or effector peptides can be delivered against pathogenic bacteria by being cloned and expressed in probiotic organisms for therapeutic delivery in vivo. Recombinant expression (and overexpression) and export of antimicrobial peptides and other peptides are well documented in bacteria, including species that are also utilized as probiotics.
In various embodiments the targeting peptides, antimicrobial peptides, and/or STAMPs can be formulated individually, in combination with each other, in combination with other antimicrobial peptides, and/or in combination with various antibacterial agents to provide antimicrobial reagents and/or pharmaceuticals.
Accordingly, in certain embodiments this invention provides peptides having antimicrobial activity, compositions comprising the peptides, methods of using the peptides (or compositions thereof) to inhibit the growth of or kill a wide variety of microbial targets and methods of using the peptides (or compositions thereof) to treat or prevent microbial infections and diseases related thereto in both plants and animals.
The various peptides (targeting peptides, AMPs, STAMPs, etc.) described herein exhibit antimicrobial activity, being biostatic or biocidal against a certain microbial targets, including but not limited to, Gram-negative bacteria such as Acinetobacter baumannii, Escherichia coli, Fusobacterium nucleatum, Pseudomonas aeruginosa, Porphyromonas gingivalis; Gram-positive bacteria such as Actinomyces naeslundii, Bacillus subtilis, Clostridium difficile, Enterococcus faecalis, Staphylococcus aureus (and MRSA), S. epidermidis, Streptococcus mutans, Streptococcus pneumoniae; and yeast or fungi such as Aspergillus niger, Candida albicans, Malassezia furfur, and Trichophyton rubrum (see, e.g., Table 2). Significantly, various peptides described herein are biostatic or biocidal against clinically relevant pathogens exhibiting multi-drug resistance such as, for example, methicillin-resistant Staphylococcus aureus (“MRSA”).
TABLE 2
Illustrative target microorganisms and associated pathology.
Acinetobacter baumannii Pathogenic gram-negative bacillus that is naturally sensitive
(A. baumannii) to relatively few antibiotics.
Actinomyces naeslundii Gram positive rod shaped bacteria that occupy the oral
(A. naeslundii) cavity and are implicated in periodontal disease and root
caries.
Aspergillus niger A fungal infection that often causes a black mould to appear
(A. niger) on some fruit and vegetables but may also infect humans
through inhalation of fungal spores.
Bacteroides fragilis Gram positive bacilli that are opportunistic human
(B. fragilis) pathogens, causing infections of the peritoneal cavity,
gastrointestinal surgery, and appendicitis via abscess
formation, inhibiting phagocytosis. Resistant to a wide
variety of antibiotics - β-lactams, aminoglycosides, and
recently many species have acquired resistance to
erythromycin and tetracycline.
Bacillus subtilis Gram-positive, catalase-positive bacterium.
(B. subtilis)
Candida albicans Causal agent of opportunistic oral and genital fungal
(C. albicans) infections in humans.
Clostridium difficile A gram-positive, anaerobic, spore-forming bacillus that is
(C. difficile) responsible for the development of antibiotic-associated
diarrhea and colitis.
Corynebacterium jeikeium Gram positive, opportunistic pathogen primarily of
(C. jeikeium) immunocompromised (neutropenic) patients. Highly
resistant to antibiotics
Campylobacter jejuni Gram negative cause of human gastroenteritis/food
(C. jejuni) poisoning.
Escherichia coli Gram negative rod-shaped bacterium commonly found in the
(E. coli) lower intestine of warm-blooded organisms. Certain strains
cause serious food poisoning in humans.
Enterococcus faecalis Gram-positive commensal bacterium
(E. faecalis)
Fusobacterium nucleatum Gram negative schizomycetes bacterium often seen in
(F. nucleatum) necrotic tissue and implicated, but not conclusively, with
other organisms in the causation and perpetuation of
periodontal disease.
Lactobacillus acidophilus Gram-positive commensal bacterium.
(L. acidophilus)
Legionella pneumophila Gram negative bacterium that is the causative agent of
(L. pneumophila) legionellosis or Legionnaires' disease.
(Micrococcus luteus) Gram positive, spherical, saprotrophic bacterium found in
M. luteus soil, dust, water and air, and as part of the normal flora of the
mammalian skin. The bacterium also colonizes the human
mouth, mucosae, oropharynx and upper respiratory tract.
Considered an emerging nosocomial pathogen in
immunocompromised patients.
Mycobacterium smegmatis Gram-variable (acid-fast) soil-dwelling organism utilized as
(M. smegmatis) a proxy for Mycobacterium tuberculosis during research and
development.
Malassezia furfur Yeast - cutaneous pathogen.
(M. furfur)
Methicillin-resistant Any strain of Staphylococcus aureus bacteria (gram positive)
Staphylococcus aureus that is resistant to a one or more members of a large group of
(MRSA) antibiotics called the beta-lactams. Responsible for skin and
systemic infections.
Myxococcus xanthus Gram negative cells that form biofilms and display primitive
(M. xanthus) social motility and fruiting body organization.
Pseudomonas aeruginosa Gram-negative rod. Frequent opportunistic pathogen and
P. aeruginosa infects burn wounds. Causes ear infections in children.
Infects the lungs of cystic fibrosis patients.
Porphyromonas gingivalis Non-motile, gram-negative, rod-shaped, anaerobic
(P. gingivalis) pathogenic bacterium (periodontal disease)
Progeussmirabilis Gram-negative, facultatively anaerobic bacterium. Causes
(P. mirabilis) 90% of all ‘Proteus’ infections in humans.
S. epidermidis Gram-positive, coagulase-negative cocci. Nosocomial
(S. epidermidis) pathogen associated with infection (biofilm) of implanted
medical device.
Streptococcus mutans Gram-positive, facultatively anaerobic bacterium commonly
(S. mutans) found in the human oral cavity and is a significant
contributor to tooth decay
Streptococcus pneumoniae Gram-positive, alpha-hemolytic, bile soluble aerotolerant
(S. pneumoniae) anaerobe. Causal agent for streptococcal pneumonia.
Treponema denticola Gram-negative oral spirochete associated with the incidence
(T. denticola) and severity of human periodontal disease.
Trichophyton rubrum Most common cause of athlete's foot, jock itch and
(T. rubrum) ringworm.
The various agents described herein (targeting peptides, compound targeting peptides, antimicrobial peptides (AMPs) and/or compound AMPs, STAMPs and/or other chimeric moieties). or compositions thereof, are useful as biocidal or biostatic or fungicidal or fungistatic agents and/or virucidal agents in a wide variety of applications. For example, the agents can be used to disinfect or preserve a variety of materials including medical instruments, foodstuffs, medicaments, cosmetics and other nutrient-containing materials. Various peptides described herein are particularly useful as bacteriostatic or bactericidal agents against multi-drug-resistant pathogens such as MRSA in a variety of clinical settings.
The agents described herein, or compositions thereof, are also useful for the prophylaxis or treatment of microbial infections and diseases related thereto in both plants and animals. Such diseases include, but are not limited to, Gram-negative and Gram-positive bacterial infections, endocarditis, pneumonia and other respiratory infections, urinary tract infections, systemic candidiasis, oral mucositis, fungal infections, biofilm formation or maintenance (e.g., on medical implants), and the like.
In various embodiments, the agents described herein can be formulated individually, in combination with each other, in combination with other antimicrobial peptides, and/or in combination with various antibiotic (e.g., antibacterial) agents in “home healthcare” formulations. Such formulations include, but are not limited to toothpaste, mouthwash, tooth whitening strips or solutions, contact lens storage, wetting, or cleaning solutions, dental floss, toothpicks, toothbrush bristles, oral sprays, oral lozenges, nasal sprays, aerosolizers for oral and/or nasal application, wound dressings (e.g., bandages), and the like.
Such applications are illustrative and not limiting. Using the teachings provided herein other uses of the AMPs and compositions described herein will be recognized by one of
I. Targeting Peptides. A) Uses of Targeting Peptides.
The novel microorganism-binding peptides (targeting peptides) described herein can be used to preferentially or specifically deliver an effector to a microorganism (e.g., a bacterium, a fungus, a protozoan, an algae, etc.), to a bacterial film, to a biofilm, and the like. The targeting peptides described herein can be used to bind to and thereby label particular targets, and/or as capture reagents to bind target microorganisms and thereby provide an indicator of the presence and/or quantity of the target microorganism(s). In certain embodiments the targeting peptide can be attached to an effector such as an epitope tag and/or a detectable label and thereby facilitate the identification of the presence and/or location, and/or quantity of the target (e.g., target organism). Thus targeting moieties are thus readily adapted for use in in vivo diagnostics, and/or ex vivo assays. Moreover, because of small size and good stability, microorganism binding peptides are well suited for microassay systems (e.g., microfluidic assays (Lab on a Chip), microarray assays, and the like).
In certain embodiments the microorganism binding peptides (targeting peptides) can be attached to an effector that has antimicrobial activity (e.g., an antimicrobial peptide, an antibacterial and/or antifungal, a vehicle that contains an antibacterial or antifungal, etc. In various embodiments these chimeric moieties can be used in vivo, or ex vivo to preferentially inhibit or kill the target organism(s).
In certain embodiments the targeting peptides can be recombinantly expressed as part of a yeast or phage tail fiber or coat protein to enhance binding of the yeast or phage to a specific bacterial Gram-designation, genus, species, or strain. Phage with expressed peptides will then display altered infection selectivity towards a designed target bacteria for use in phage therapy. Cloning the DNA encoding a peptide of interest into the major or minor coat proteins of a bacteriophage, for example in Proteins I through VIII of phages SAP-2, M13, or T7, will result in a targeted phage expressing 1-200 copies of the targeting peptide on the phage surface.
In certain embodiments the targeting peptides can be used in various pre-targeting p rotocols. In pre-targeting protocols, a chimeric molecule is utilized comprising a primary targeting species (e.g. a microorganism-binding peptide) that specifically binds the desired target (e.g. a bacterium) and an effector that provides a binding site that is available for binding by a subsequently administered second targeting species. Once sufficient accretion of the primary targeting species (the chimeric molecule) is achieved, a second targeting species comprising (i) a diagnostic or therapeutic agent and (ii) a second targeting moiety, that recognizes the available binding site of the primary targeting species, is administered.
An illustrative example of a pre-targeting protocol is the biotin-avidin system for administering a cytotoxic radionuclide to a tumor. In a typical procedure, a monoclonal antibody targeted against a tumor-associated antigen is conjugated to avidin and administered to a patient who has a tumor recognized by the antibody. Then the therapeutic agent, e.g., a chelated radionuclide covalently bound to biotin, is administered. The radionuclide, via its attached biotin is taken up by the antibody-avidin conjugate pretargeted at the tumor. Examples of pre-targeting biotin/avidin protocols are described, for example, in Goodwin et al., U.S. Pat. No. 4,863,713; Goodwin et al. (1988) J. Nucl. Med. 29: 226; Hnatowich et al. (1987) J. Nucl. Med. 28: 1294; Oehr et al. (1988) J. Nucl. Med. 29: 728; Klibanov et al. (1988) J. Nucl. Med. 29: 1951; Sinitsyn et al. (1989) J. Nucl. Med. 30: 66; Kalofonos et al. (1990) J. Nucl. Med. 31: 1791; Schechter et al. (1991) Int. J. Cancer 48:167; Paganelli et al. (1991) Cancer Res. 51: 5960; Paganelli et al. (1991) Nucl. Med. Commun. 12: 211; Stickney et al. (1991) Cancer Res. 51: 6650; and Yuan et al. (1991) Cancer Res. 51:3119.
It will be recognized that the tumor-specific antibody used for cancer treatments can be replaced with a microorganism binding peptide of the present invention and similar pre-targeting strategies can be used to direct labels, antibiotics, and the like to the target organism(s).
Three-step pre-targeting protocols in which a clearing agent is administered after the first targeting composition has localized at the target site also have been described. The clearing agent binds and removes circulating primary conjugate which is not bound at the target site, and prevents circulating primary targeting species (antibody-avidin or conjugate, for example) from interfering with the targeting of active agent species (biotin-active agent conjugate) at the target site by competing for the binding sites on the active agent-conjugate. When antibody-avidin is used as the primary targeting moiety, excess circulating conjugate can be cleared by injecting a biotinylated polymer such as biotinylated human serum albumin. This type of agent forms a high molecular weight species with the circulating avidin-antibody conjugate which is quickly recognized by the hepatobiliary system and deposited primarily in the liver.
Examples of these protocols are disclosed, e.g., in PCT Application No. WO 93/25240; Paganelli et al. (1991) Nucl. Med. Comm., 12: 211-234; Oehr et al. (1988) J. Nucl. Med., 29: 728-729; Kalofonos et al. (1990) J. Nucl. Med., 31: 1791-1796; Goodwin et al. (1988) J. Nucl. Med., 29: 226-234; and the like).
These applications of microorganism binding peptides of this invention are intended to be illustrative and not limiting. Using the teaching provided herein, other uses will be recognized by one of skill in the art.
B) Illustrative Novel Targeting Peptides.
In certain embodiments, the targeting moiety comprises one or more targeting peptides that bind particular bacteria, fungi, and/or yeasts, and/or algae, and/or viruses and/or that bind particular groups of bacteria, and/or groups of fungi, and/or groups of yeasts, and/or groups of algae.
In certain embodiments the targeting peptides include peptides comprising or consisting of one or more of the amino acid sequences shown in Table 3 (SEQ ID NOs:13-1566). In various embodiments the peptides include peptides comprising or consisting of the retro, inverso, retro-inverso, and/or beta form of one or more of the amino acid sequences shown in Table 3. Also contemplated are circular permutations of these sequences as well as peptides comprising or consisting of the retro, inverso, retro-inverso, and/or beta form of such circular permutations.
It will also be recognized, that in certain embodiments, any peptide or compound AMP described herein can be circularized.
In various embodiments the peptides can optionally bear one or more protecting groups, e.g., and the amino and/or carboxyl termini, and/or on side chains.
Also contemplated are peptides comprising one, two, three four, or five conservative substitutions of these amino acid sequences.
TABLE 3
Illustrative list of novel targeting peptides.
SEQ ID
ID Target(s) Targeting Peptide Sequence NO
1T-3 S. mutans VLGIAGGLDAYGELVGGN 13
S. gordonii
1T-4 S. mutans LDAYGELVGGN 14
S. gordonii
S. sanguinis
S. oralis
V. atypica
L. casei
1T-6 S. mutans KFINGVLSQFVLERK 15
1T-7 M. xanthus SQRIIEPVKSPQPYPGFSVS 16
1T-8 M. xanthus FSVAACGEQRAVTFVLLIEDLI 17
1T-9 M. xanthus WAWAESPRCVSTRSNIHALAFRVEVAA 18
LT
1T-10 M. xanthus SPAGLPGDGDEA 19
1T-11 S. mutans RISE 20
S. epidermidis
P. aeruginosa
1T-12 C. xerosis FGNIFKGLKDVIETIVKWTAAK 21
C. striatum
S. epidermidis
S. mutans
1T-13 S. aureus FRSPCINNNSLQPPGVYPAR 22
S. epidermidis
P. aeruginosa
1T-14 S. mutans ALAGLAGLISGK 23
S. aureus
S. epidermidis
C. xerosis
1T-15 S. mutans DVILRVEAQ 24
1T-16 P. aeruginosa IDMR 25
1T-17 S. mutans NNAIVYIS 26
1T-18 S. aureus YSKTLHFAD 27
S. epidermidis
C. striatum
P. aeruginosa
1T-19 S. aureus PGAFRNPQMPRG 28
S. epidermidis
P. aeruginosa
1T-20 S. mutans PALVDLSNKEAVWAVLDDHS 29
P. aeruginosa
1T-21 S. mutans YVEEAVRAALKKEARISTEDTPVNLPSF 30
P. aeruginosa DC
1T-22 S. epidermidis VPLDDGTRRPEVARNRDKDRED 31
P. aeruginosa
1T-23 S. mutans PALVDLSNKEAVWAVLDDHS 32
P. aeruginosa
1T-24 P. aeruginosa EEAEEKLAEVSQAVKRLVR 33
1T-25 S. aureus VGLDVSVLVLFFGLQLLSVLLGAMIR 34
S. epidermidis
C. xerosis
C. striatum
P. aeruginosa
1T-26 S. mutans LTILPTTFFAIIVPILAVAFIAYSGFKIKGI 35
S. aureus VEHKDQW
S. epidermidis
C. jeikeium
C. xerosis
C. striatum
P. aeruginosa
1T-27 S. mutans ALFVSLEQFLVVVAKSVFALCHSGTLS 36
S. aureus
S. epidermidis
C. jeikeium
C. xerosis
C. striatum
P. aeruginosa
1T-28 P. aeruginosa VSRDEAMEFIDREWTTLQPAGKSHA 37
1T-29 S. mutans GSVIKKRRKRMSKKKHRKMLRRTRVQ 38
S. aureus RRKLGK
S. epidermidis
C. jeikeium
C. xerosis
C. striatum
P. aeruginosa
1T-30 S. aureus GKAKPYQVRQVLRAVDKLETRRKKGGR 39
S. epidermidis
C. xerosis
C. striatum
P. aeruginosa
1T-31 S. mutans NATGTDIGEVTLTLGRFS 40
P. aeruginosa
1T-32 S. mutans VSFLAGWLCLGLAAWRLGNA 41
1T-33 S. aureus VRTLTILVIFIFNYLKSISYKLKQPFENNL 42
S. epidermidis AQSMISI
C. jeikeium
C. xerosis
C. striatum
P. aeruginosa
1T-34 S. aureus AFWLNILLTLLGYIPGIVHAVYIIAKR 43
S. epidermidis
C. jeikeium
C. xerosis
C. striatum
P. aeruginosa
1T-35 P. aeruginosa EICLTLVFPIRGSYSEAAKFPVPIHIVEDG 44
TVELPK
1T-36 S. aureus VYRHLRFIDGKLVEIRLERK 45
S. epidermidis
C. jeikeium
C. xerosis
C. striatum
P. aeruginosa
1T-37 S. mutans YIVGALVILAVAGLIYSMLRKA 46
S. aereus
S. epidermidis
C. jeikeium
C. xerosis
C. striatum
P. aeruginosa
1T-38 S. mutans VMFVLTRGRSPRPMIPAY 47
S. aereus
S. epidermidis
C. jeikeium
C. xerosis
C. striatum
P. aeruginosa
1T-39 S. mutans FGFCVWMYQLLAGPPGPPA 48
P. aeruginosa
1T-40 S. mutans QRVSLWSEVEHEFR 49
P. aeruginosa
1T-41 S. mutans KRGSKIVIAIAVVLIVLAGVWVW 50
S. aureus
S. epidermidis
C. jeikeium
C. striatum
P. aeruginosa
1T-42 S. aureus TVLDWLSLALATGLFVYLLVALLRADRA 51
S. epidermidis
C. xerosis
C. striatum
P. aeruginosa
1T-43 C. jeikium DRCLSVLSWSPPKVSPLI 52
P. aeruginosa
1T-44 S. mutans DPALADFAAGMRAQVRT 53
S. aureus
S. epidermidis
C. jeikeium
C. striatum
P. aeruginosa
1T-45 S. aureus WTKPSFTDLRLGFEVTLYFANR 54
S. epidermidis
C. striatum
P. aeruginosa
1T-46 S. aureus FSFKQRVMFRKEVERLR 55
S. epidermidis
C. jeikeium
C. xerosis
C. striatum
P. aeruginosa
1T-47 S. mutans VIKISVPGQVQMLIP 56
S. epidermidis
P. aeruginosa
1T-48 S. aureus KLQVHHGRATHTLLLQPPLCAPGTIR 57
S. epidermidis
C. jeikeium
C. xerosis
C. striatum
P. aeruginosa
1T-49 S. aureus SLVRIHDQQPWVTRGAFIDAARTCS 58
S. epidermidis
C. jeikeium
P. aeruginosa
1T-50 P. aeruginosa HSDEPIPNILFKSDSVH 59
1T-51 S. aureus GKPKRMPAEFIDGYGQALLAGA 60
P. aeruginosa
1T-52 S. aureus DEYPAKLPLSDKGATEPRRH 61
C. xerosis
P. aeruginosa
1T-53 P. aeruginosa SDILAEMFEKGELQTLVKDAAAKANA 62
1T-54 S. epidermidis RWVSCNPSWRIQ 63
C. xerosis
C. striatum
P. aeruginosa
1T-55 C. xerosis NHKTLKEWKAKWGPEAVESWATLLG 64
P. aeruginosa
1T-56 C. xerosis LALIGAGIWMIRKG 65
P. aeruginosa
1T-57 P. aeruginosa RLEYRRLETQVEENPESGRRPMRG 66
1T-58 P. aeruginosa CDDLHALERAGKLDALLSA 67
1T-59 S. aureus AVGNNLGKDNDSGHRGKKHRKHKHR 68
S. epidermidis
P. aeruginosa
1T-60 S. aureus YLTSLGLDAAEQAQGLLTILKG 69
S. epidermidis
C. jeikeium
C. striatum
P. aeruginosa
1T-61 P. aeruginosa HATLLPAVREAISRQLLPALVPRG 70
1T-62 S. epidermidis GCKGCAQRDPCAEPEPYFRLR 71
P. aeruginosa
1T-63 S. aureus EPLILKELVRNLFLFCYARALR 72
S. epidermidis
C. jeikeium
C. xerosis
C. striatum
P. aeruginosa
1T-64 S. aureus QTVHHIHMHVLGQRQMHWPPG 73
S. epidermidis
C. jeikeium
C. xerosis
C. striatum
P. aeruginosa
1T-65 S. mutans HARAAVGVAELPRGAAVEVELIAAVRP 74
S. aureus
S. epidermidis
C. jeikeium
C. xerosis
C. striatum
P. aeruginosa
1T-66 S. mutans DTDCLSRAYAQRIDELDKQYAGIDKPL 75
S. aureus
S. epidermidis
C. jeikeium
C. xerosis
C. striatum
P. aeruginosa
1T-67 S. aureus GQRQRLTCGRVSGCSEGPSREAAR 76
S. epidermidis
C. jeikeium
C. xerosis
C. striatum
P. aeruginosa
1T-68 S. mutans GGTKEIVYQRG 77
S. aureus
C. jeikeium
C. xerosis
C. striatum
P. aeruginosa
1T-69 S. mutans ILSQEADRKKLF 78
P. aeruginosa
1T-70 S. aureus NRQAQGERAHGEQQG 79
C. jeikeium
P. aeruginosa
1T-71 P. aeruginosa KIDTNQWPPNKEG 80
1T-72 P. aeruginosa EPTDGVACKER 81
1T-73 S. pneumoniae GWWEELLHETILSKFKITKALELPIQL 82
1T-74 S. pneumoniae DIDWGRKISCAAGVAYGAIDGCATTV 83
1T-75 S. pneumoniae GVARGLQLGIKTRTQWGAATGAA 84
1T-76 S. pneumoniae EMRLSKFFRDFILWRKK 85
1T-77 S. pneumoniae EMRISRIILDFLFLRKK 86
1T-78 S. pneumoniae FFKTIFVLILGALGVAAGLYIEKNYIDK 87
1T-79 S. pneumoniae FGTPWSITNFWKKNFNDRPDFDSDRRRY 88
1T-80 S. pneumoniae GGNLGPGFGVIIP 89
1T-81 S. pneumoniae AIATGLDIVDGKFDGYLWA 90
1T-82 S. pneumoniae FGVGVGIALFMAGYAIGKDLRKKFGKSC 91
1T-83 S. pneumoniae QKPRKNETFIGYIQRYDIDGNGYQSLPC 92
PQN
1T-84 S. pneumoniae FRKKRYGLSILLWLNAFTNLVNSIHAFY 93
MTLF
1T-85 A. naeslundii VMASLTWRMRAASASLPTHSRTDA 94
F. nucleatum
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-86 S. mitis HRKNPVLGVGRRHRAHNVA 95
S. oralis
S. salivarious
1T-87 S. mitis EAVGQDLVDAHHP 96
S. mutans
S. oralis
1T-89 S. mitis HEDDKRRGMSVEVLGFEVVQHEE 97
S. mutans
1T-90 S. gordonii RNVIGQVL 98
S. mitis
S. mutans
S. oralis
S. sanguinis
1T-91 S. mitis TSVRPGAAGAAVPAGAAGAAGAGWR 99
S. mutans WP
S. oralis
S. sanguinis
1T-92 S. mitis GQDEGQRRAGVGEGQGVDG 100
S. mutans
1T-93 S. epidermidis AMRSVNQA 101
S. gordonii
S. mitis
S. mutans
S. oralis
S. sanguinis
1T-94 S. mitis DQVAHSGDMLVQARRRDS 102
S. mutans
S. oralis
1T-95 S. gordonii GHLLRVGGRVGGVGGVAGACAQPFGGQ 103
S. mitis
S. mutans
S. oralis
S. sanguinis
1T-96 S. gordonii VAGACAQPFGGQ 104
S. mitis
S. mutans
S. oralis
S. sanguinis
1T-97 A. naeslundii GVAERNLDRITVAVAIIWTITIVGLGLV 105
F. nucleatum AKLG
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-98 A. naeslundii VRSAKAVKALTAAGYTGELVNVSGGM 106
F. nucleatum KAWLGQ
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-99 S. gordonii MKAWLGQ 107
S. mitis
S. mutans
S. oralis
S. sanguinis
1T-100 S. gordonii LDPLEPRIAPPGDRSHQGAPACHRDPLR 108
S. mitis GRSARDAER
S. mutans
1T-101 A. naeslundii RLRVGRATDLPLTSFAVGVVRNLPDAP 109
P. gingivalis AH
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. sanguinis
1T-102 A. naeslundii WKRLWPARILAGHSRRRMRWMVVWR 110
F. nucleatum YFAAT
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-103 A. naeslundii AQFYEAIITGYALGAGQRIGQL 111
F. nucleatum
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. sanguinis
1T-104 S. mitis RAVAAHLQGRHHGHQVRRQRHGQR 112
1T-105 S. epidermidis GEGLPPPVLHLPPPRMSGR 113
S. gordonii
S. mitis
S. mutans
S. oralis
1T-106 S. gordonii DALRRSRSQGRRHR 114
S. mitis
S. mutans
S. oralis
S. salivarious
1T-107 A. naeslundii SPVPRFTAVGGVSRGSP 115
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-108 S. gordonii WGPLGPERPLW 116
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-109 A. naeslundii VTTNVRQGAGS 117
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-110 A. naeslundii LAAKTAVCVGRAFM 118
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. sanguinis
1T-111 A. naeslundii GRLSRREEDPATSIILLRGAYRMAVF 119
F. nucleatum
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-112 S. gordonii SDNDGKLILGTSQ 120
1T-113 S. mitis HGAHQRTGQRLHHHRGRTVSGCRQNP 121
VAGVDPDEHR
1T-114 A. naeslundii RQAPGPGLVTITAACSAPGSRSR 122
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. sanguinis
1T-115 A. naeslundii LLIERFSNHH 123
F. nucleatum
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-116 A. naeslundii MILHRRRDR 124
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-117 S. mutans GPGVVGPAPFSRLPAHALNL 125
1T-118 A. naeslundii TASPPAPSDQGLRTAFPATLLIALAALA 126
F. nucleatum RISR
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-119 S. gordonii SPATQKAPTRAQPSRAPVQDCGDGRPT 127
S. mitis AAPDDVERLSPR
S. mutans
S. oralis
1T-120 A. naeslundii DVRDRVDLAGADLCAAHATR 128
F. nucleatum
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-121 S. gordonii FAKETGFGIGGAQEGWWIIADIYGPNPF 129
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-122 S. mitis GAIPDPVTHRVDWEEDHQTRPSR 130
1T-123 S. gordonii LVRRNAVAGRSDGLAGAEQLDLVRLQ 131
GVL
1T-124 S. mitis LFDERNKIA 132
S. mutans
S. oralis
1T-125 S. epidermidis DAITGGNPPLSDTDGLRP 133
S. gordonii
S. mutans
S. oralis
1T-126 S. gordonii QGLARPVLRRIPL 134
S. mitis
S. mutans
1T-127 A. naeslundii YDPVPKRKNKNSEGKREE 135
F. nucleatum
P. gingivalis
T. denticola
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-128 A. naeslundii SGSAIRMLEIATKMLKR 136
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-129 A. naeslundii YDKYIKYLSIQPPFIVYFI 137
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-130 A. naeslundii QKIIDMSKFLFSLILFIMIVVIYIGKSIGG 138
F. nucleatum YSAIVSSIMLELDTVLYNKKIFFIYK
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-131 A. naeslundii DEVWKMLGI 139
F. nucleatum
P. gingivalis
T. denticola
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-132 A. naeslundii YSKKLFEYFYFIIFILIRYLIFYKIIQNKNY 140
F. nucleatum YINNIAYN
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-133 A. naeslundii YFIKDDNEALSKDWEVIGNDLKGTIDK 141
P. gingivalis YGKEFKVR
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-134 A. naeslundii SRLVREIKKKCRKS 142
F. nucleatum
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-135 A. naeslundii FESLLPQATKKIVNNKGSKINKIF 143
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-136 A. naeslundii ELLTQIRLALLYSVNEW 144
F. nucleatum
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-137 A. naeslundii PLNFYRAVKENRLPLSEKNINDFTNIKL 145
F. nucleatum KVSPKLINLLQESSIFYNFSPKKRNTN
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-138 A. naeslundii YPNEYCIFLENLSLEELKEIKAINGETLN 146
F. nucleatum LEEIINERKNLKD
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-139 A. naeslundii AVAGAAVGALLGNDARSTAVGAAIGG 147
S. gordonii ALGAGAGELTKNK
S. mitis
S. mutans
S. oralis
1T-140 A. naeslundii IKGTIAFVGEDYVEIRVDKGVKLTFRKS 148
F. nucleatum AIANVINNNQQ
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-141 F. nucleatum KKFIILLFILVQGLIFSATKTLSDIIAL 149
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. sanguinis
1T-142 A. naeslundii FTQGIKRIVLKRLKED 150
F. nucleatum
P. gingivalis
T. denticola
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-143 A. naeslundii MPKRHYYKLEAKALQFGLPFAYSPIQL 151
F. nucleatum LK
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-144 A. naeslundii IIELHPKSWTQDWRCSFL 152
F. nucleatum
P. gingivalis
T. denticola
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-145 S. mitis VEAGKRNISLENIEKISKGLGISISELFKY 153
S. mutans IEEGEDKIG
S. oralis
1T-146 A. naeslundii RNSADNQTKIDKIRIDISLWDEHLNIVK 154
F. nucleatum QGK
P. gingivalis
T. denticola
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-147 A. naeslundii GVENRRFYERDVSKVSMMTSEAVAPR 155
F. nucleatum GGSK
P. gingivalis
T. denticola
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-148 A. naeslundii IVELDDTTILERALSMLGEANA 156
F. nucleatum
P. gingivalis
T. denticola
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-149 A. naeslundii SVRAVKPIDETVARHFPGDFIVN 157
F. nucleatum
P. gingivalis
T. denticola
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-150 A. naeslundii YINRRLKKAFSDADIKEAPAEFYEELRR 158
F. nucleatum VQYV
P. gingivalis
T. denticola
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-151 A. naeslundii SVRAVKPIDEIVAWHFPGDFIVN 159
F. nucleatum
P. gingivalis
T. denticola
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-152 A. naeslundii YVSADESAYNHIVTDDIPLADRRIEAVQQ 160
F. nucleatum
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-153 A. naeslundii YIACPGYFY 161
F. nucleatum
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-154 P. gingivalis YFSFLEIVGMARR 162
1T-155 A. naeslundii LKLAFGVYPFQAMSQSDTAVSERNVL 163
F. nucleatum WR
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-156 A. naeslundii GRFQISIRGEEKSKVKVQGKGTFTDRNTT 164
F. nucleatum
P. gingivalis
T. denticola
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-157 A. naeslundii RRFRKTTENREKSKNKKAVLGLSTTST 165
F. nucleatum ASY
P. gingivalis
T. denticola
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-158 A. naeslundii WENKPSPLGSIKKLQGLVYRLIGYRHF 166
F. nucleatum WV
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-159 P. gingivalis IFSLHHFALICSEMGTFAVSKRAKYKWE 167
VL
1T-160 A. naeslundii AQYKYINKLLN 168
F. nucleatum
P. gingivalis
T. denticola
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-161 A. naeslundii NKVLQVEVMWDGSVVGRPAGVISIKSS 169
F. nucleatum KKG
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-162 A. naeslundii QKAKEESDRKAAVSYNGFHRVNVVSIPK 170
F. nucleatum
P. gingivalis
T. denticola
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-163 A. naeslundii MENILIYIPMVLSPFGSGILLFLGKDRRY 171
F. nucleatum ML
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-164 A. naeslundii KKSHSQGKRKLKDLNSAYKIDNQLHYA 172
F. nucleatum LR
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-165 A. naeslundii CYDSFDFSIFVTFANRMKLSVGS 173
F. nucleatum
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-166 A. naeslundii AQSAGQIKRKSKVRIHV 174
F. nucleatum
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-167 A. naeslundii SRMSEHSPAGLVFEVGPMDKGSFIILDS 175
F. nucleatum YHPTVKK
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-168 A. naeslundii ELHRIMSTEKIGAVTKMNFDTAPIMSILP 176
F. nucleatum IDIYPKEVGIGS
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-169 A. naeslundii FARVRRLHQNRILTQPLTNLKYCLRQPI 177
F. nucleatum YSD
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-170 P. gingivalis AYGKVFSMDIMLSENDKLIVLRISHHSA 178
WH
1T-171 A. naeslundii SVRAVKPIDKTVARHFPGDFIVN 179
F. nucleatum
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-172 A. naeslundii FEGLKNLLGDDII 180
F. nucleatum
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-173 A. naeslundii LFRKEDQEHVLL 181
F. nucleatum
P. gingivalis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-174 A. naeslundii SGGSDTDGSSSGEPGSHSGDL 182
F. nucleatum
P. gingivalis
T. denticola
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-175 A. naeslundii GEPGSHSGDL 183
F. nucleatum
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-176 A. naeslundii PVGDIMSGFLRGANQPRFLLDHISFGS 184
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-177 P. gingivalis GTNVPTQILGYSREERFDYEPAPEQR 185
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-178 A. naeslundii LLASHPERLSLGVFFVYRVLHLLLENT 186
F. nucleatum
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-179 A. naeslundii TCYPLIQRKTDRAYEA 187
F. nucleatum
P. gingivalis
T. denticola
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-180 A. naeslundii VVFGGGDRLV 188
F. nucleatum
P. gingivalis
T. denticola
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-181 A. naeslundii YGKESDP 189
F. nucleatum
P. gingivalis
T. denticola
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-182 A. naeslundii LTASICRQWNDNSTPYQR 190
F. nucleatum
P. gingivalis
T. denticola
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-183 A. naeslundii PLRSFVAEKAEHAFRVVRIADFDFGHS 191
F. nucleatum
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-184 A. naeslundii ALLVLNLLLMQFFFGKNM 192
F. nucleatum
P. gingivalis
T. denticola
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-185 A. naeslundii HYHFLLEFGFHKGDYLE 193
F. nucleatum
P. gingivalis
T. denticola
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-188 S. sanguinis HRKDVYKK 194
1T-190 A. naeslundii IQIIVNAFVEKDKTGAVIEVLYASNNHE 195
F. nucleatum KVKAKYEELVAIS
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-192 S. sanguinis ILVLLALQVELDSKFQY 196
1T-193 S. sanguinis LMIFDKHANLKYKYGNRSFGVEAIM 197
1T-195 S. mutans AASGFTYCASNGVWHPY 198
1T-196 F. nucleatum KPEKEKLDTNTLMKVVNKALSLFDRLL 199
S. sanguinis IKFGA
1T-197 A. naeslundii TEILNFLITVCADRENWKIKHGLSDSVL 200
F. nucleatum LIFFARFTGAEYW
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-198 P. gingivalis MPVSKKRYMLSSAYATALGICYGQVAT 201
S. epidermidis DEKESEITAIPDLLDYLSVEEYLL
S. gordonii
S. mitis
S. mutans
S. oralis
S. sanguinis
1T-199 S. sanguinis RAGRIKKLSQKEAEPFEN 202
1T-200 A. naeslundii MRFKRFDRDYALSGDNVFEVLTASCDV 203
F. nucleatum IERNLSYREMCGLMQ
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-201 S. sanguinis KRKHENVIVAEEMRVIKN 204
1T-202 A. naeslundii LCRLEKLCKQFLRQDKVVTYYLMLPYK 205
F. nucleatum RAIEAFYQELKERS
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-203 A. naeslundii YPFCLATVDHLPEGLSVTDYERVQRLV 206
F. nucleatum SQFLLNKEER
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-207 F. nucleatum SPLEKYGTGSMTALTFLLGCCLLVLSKK 207
S. sanguinis SR
1T-208 Unanalyzed KRKRWAILTLFLAGLGAVGIVLATF 208
1T-215 S. sanguinis VCFKDISVFLSPFRGQEVLFCGKAKHSL 209
IYVIGT
1T-216 S. sanguinis FFLNVIAIRIPHF 210
1T-217 F. nucleatum MLSNVLSRSVVSPNVDIPNSMVILSPLLI 211
S. sanguinis SISNYH
1T-218 F. nucleatum KLIFAALGLVFLLIGLRDSRSK 212
S. sanguinis
1T-219 S. sanguinis RNINVSATFITEKSLV 213
1T-221 A. naeslundii DIGRIIGKKGRTITAIRSIVYSVPTQGKK 214
F. nucleatum VRLVIDEK
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-222 F. nucleatum RIEASLISAIMFSMFNAIVKFLQK 215
S. sanguinis
1T-223 A. naeslundii NQKMEINSMTSEKEKMLAGHFHNEAN 216
F. nucleatum FAVIFKYSLFYNFF
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-225 A. naeslundii RRSLGNSASFAEWIEYIRYLHYIIRVQFI 217
F. nucleatum HFFSKNKKI
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-226 A. naeslundii KLQEKQIDRNFERVSGYSTYRAVQAAK 218
F. nucleatum AKEKGFISLEN
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-228 A. naeslundii IFKLFEEHLLYLLDAFYYSKIFRRLKQGL 219
F. nucleatum YRRKEQPYTQDLFRM
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-230 A. naeslundii EFLEKFKVLKQPRKANNISKNRVAMIFL 220
F. nucleatum TIHKSRGFLSSPY
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-233 A. naeslundii TDQELEHLIVTELESKRLDFTYSKDITEF 221
P. gingivalis FDEAFPEYDQNY
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-234 A. naeslundii DNFYLILKMEERGKSKKTSQTRGFRAFF 222
F. nucleatum DIIRKKIKKEDGK
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-237 S. sanguinis EDPVPNHFTLRRNKKEKPSKS 223
1T-238 A. naeslundii IFNRRKFFQYFGLSKEAMVEHIQPFILDI 224
F. nucleatum WQIHLF
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-239 A. naeslundii ADDLLNKRLTDLIMENAETVKTIDLDN 225
S. gordonii SD
S. mitis
S. mutans
S. oralis
S. sanguinis
1T-240 A. naeslundii VILGNGISNIAQTLGQLPNIAWVWIYMV 226
F. nucleatum LIAALLEESNVC
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-242 F. nucleatum KQVQNTTLIICGTVLLGILFKSYLKSQKSV 227
S. sanguinis
1T-243 A. naeslundii SENIARFAAAFENEQVVSYARWFRRSW 228
P. gingivalis RGSGSSSRF
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-248 S. sanguinis IGGALNSCG 229
1T-249 F. nucleatum VFSVLKHTTWPTRKQSWHDFISILEYSA 230
S. sanguinis FFALVIFIFDKLLTLGLAELLKRF
1T-250 S. mitis LVQGDTILIENHVGTPVKDDGKDCLIIR 231
S. mutans EADVLAVVND
S. oralis
1T-252 F. nucleatum MKKNLKRFYALVLGFIIGCLFVSILIFIGY 232
S. sanguinis
1T-253 A. naeslundii KTKESLTQQEKKFLKDYDRKSLHHFRD 233
F. nucleatum ILTYCFILDKLTNK
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-256 S. sanguinis KGKSLMPLLKQINQWGKLYL 234
1T-257 A. naeslundii IILAKAADLAEIERIISEDPFKINEIANYDI 235
F. nucleatum IEFCPTKSSKAFEKVLK
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-258 A. naeslundii TINIDDKVLDYLKKINSKAITIDLIGCAS 236
F. nucleatum
P. gingivalis
T. denticola
S. mitis
S. mutans
S. oralis
1T-259 F. nucleatum EKLKKILLKLAVCGKAWYTL 237
P. gingivalis
T. denticola
S. mitis
S. mutans
S. oralis
S. sanguinis
1T-260 A. naeslundii NILYFIHDENQWEPQKAEIFRGSIKHCA 238
P. gingivalis WLSS
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. sanguinis
1T-261 F. nucleatum SFEKNKIENNLKIAQAYIYIKPKPRICQA 239
S. mutans
S. oralis
S. sanguinis
1T-262 A. naeslundii LSLPLIVLTKSI 240
F. nucleatum
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-263 A. naeslundii FIAVSFTGNPATFKLVIGCKADN 241
F. nucleatum
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. oralis
S. salivarious
S. sanguinis
1T-264 S. sanguinis LEGKFYMAEDFDKTPECFKDYV 242
1T-265 A. naeslundii GMFENLLMINFQIMNDLKIEIVVKDRIC 243
F. nucleatum AV
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-266 S. sanguinis RAGTWLVVDEIR 244
1T-267 A. naeslundii RIKEERKNRSYKFFIWRLFDEKTGFI 245
F. nucleatum
P. gingivalis
T. denticola
S. mitis
S. mutans
S. oralis
S. sanguinis
1T-268 F. nucleatum PITPKKEKCGLGTYAPKNPVFSKSRV 246
S. mutans
S. oralis
S. sanguinis
1T-269 F. nucleatum PLYVAAVEKINTAKKH 247
S. mutans
S. oralis
S. sanguinis
1T-270 F. nucleatum VHEFDIQKILQNR 248
S. mutans
S. oralis
S. sanguinis
1T-271 A. naeslundii FLIQKFLLIKTFPPYRKKYVVIVSQTGTA 249
F. nucleatum
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-272 F. nucleatum QLAPIDKQLKAVKKIAFYESESTAAKAV 250
S. mutans TVA
S. oralis
S. sanguinis
1T-273 F. nucleatum YNEPNYKWLESYKIYKQRCEDRTGMY 251
P. gingivalis YTEET
T. denticola
S. mitis
S. mutans
S. oralis
1T-274 F. nucleatum ETTTEINAIKLHRIKQRSPQGTRRVN 252
S. mutans
S. oralis
S. sanguinis
1T-275 A. naeslundii QVLKNFSISRRYKINNPFFKILLFIQLRTL 253
F. nucleatum
P. gingivalis
T. denticola
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-276 A. naeslundii ILTLLILGSIGFFILKIKLKLGRF 254
F. nucleatum
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. sanguinis
1T-277 A. naeslundii IYYMRFVNKPLEKTFFKI 255
F. nucleatum
P. gingivalis
T. denticola
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-278 A. naeslundii SINSSAGIQPHCLSSSFVLRTKHCFY 256
F. nucleatum
P. gingivalis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-279 A. naeslundii FVLRTKHCFY 257
F. nucleatum
P. gingivalis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-280 A. naeslundii TNNKNKVIIKAIKFKNKDFINLDLFIYRR 258
F. nucleatum
P. gingivalis
T. denticola
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-281 A. naeslundii KYEKLTKENLFIRNSGNMCVFIYFLFFG 259
F. nucleatum
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-282 F. nucleatum ISLVFPAYT 260
P. gingivalis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-283 A. naeslundii LCTKLEDKQRGRIPAELFIISPIKILERND 261
F. nucleatum AL
P. gingivalis
T. denticola
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-284 A. naeslundii FQYYFSLKRV 262
F. nucleatum
P. gingivalis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-285 A. naeslundii FFPYYLADFYKQLKFLNEYQTKNKDKV 263
F. nucleatum VEFK
P. gingivalis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-286 S. sanguinis LGFFNNKADLVKADTERDNRMSSLKIK 264
DL
1T-287 P. gingivalis KGYPLPFQYRLNNH 265
T. denticola
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-288 F. nucleatum RWVGGEPSADIYLSAKDTKT 266
S. gordonii
S. salivarious
S. sanguinis
1T-289 F. nucleatum EPSADIYLSAKDTKT 267
P. gingivalis
S. gordonii
S. mitis
S. mutans
S. oralis
S. sanguinis
1T-290 A. naeslundii IINQLNLILLRLMEILIL 268
F. nucleatum
P. gingivalis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-291 A. naeslundii DMKIIKLYIKILSFLFIKYCNKKLNSVKL 269
F. nucleatum KA
P. gingivalis
T. denticola
S. mitis
S. mutans
S. oralis
1T-292 A. naeslundii IINQLNLILLRLMEILIL 270
F. nucleatum
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-293 A. naeslundii HVEDCFLLSNARTTAIHGRANPARGEPR 271
F. nucleatum TRSE
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-294 T. denticola YDKIADGVFKIGKRGVL 272
1T-295 S. mitis KYKLKKIIL 273
S. salivarious
S. sanguinis
1T-296 A. naeslundii EYSQQSFKAKPCSERGVLSP 274
F. nucleatum
P. gingivalis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-297 A. naeslundii RSLRLNNALTKLPKLWYNRIKEAFYAY 275
F. nucleatum NDYDK
T. denticola
S. mitis
S. mutans
S. oralis
1T-298 A. naeslundii ILNKKPKLPLWKLGKNYFRRFYVLPTFLA 276
F. nucleatum
P. gingivalis
T. denticola
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-299 A. naeslundii SMLTSFLRSKNTRSLKMYKDVHF 277
F. nucleatum
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-300 A. naeslundii PLIISKAQIKMSGDILGSCFKLFYLRPFF 278
F. nucleatum
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-301 F. nucleatum SKLPRVLDASLKL 279
S. gordonii
S. sanguinis
1T-302 A. naeslundii IIIILPKIYLVCKTV 280
P. gingivalis
S. epidermidis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-303 A. naeslundii LDYENMDCKKRIRI 281
F. nucleatum
P. gingivalis
S. gordonii
S. mitis
S. mutans
S. oralis
S. salivarious
S. sanguinis
1T-304 P. gingivalis STAGEASRRTASEASRRTAAKLRG 282
TT-305 F. nucleatum ARNALNMRDVPVDAAIIGIIDGMDEE 283
TT-306 F. nucleatum KILNEAEGKLLKVIEKNGEIDIEEI 284
TT-307 F. nucleatum NGDKKAKEELDKWDEVIKELNIQF 285
TT-308 F. nucleatum GLVIIPNLIALIILFSQVRQQTKDYFSNPK 286
LSSR
TT-309 F. nucleatum EPLPLTKYDKKDTEMKKVFKEILAGKV 287
GYEKEEE
TT-310 F. nucleatum TKLKKNNKLLSAKKENTLHTKDK 288
TT-311 S. mutans AIFDAMHNL 289
S. sobrinus
PVCFBP2461 P. fluorescens DLys-Dorn-Gly-DThr-Thr-Gln-Gly-DSer- 290
cDOrn
CHA0 P. fluorescens Asp-DOrn-Lys-c(Thr-Ala-Ala-DOrn-Lys) 291
CFBP2461 P. putida Asp-Lys-DAsp-Ser-DThr-DAla-Thr-DLys- 292
cOrn
NCPPB2192 P. tolaasii DSer-Lys-Ser-DSer-Thr-DSer-Orn-Thr- 293
DSer-cDOrn
PyC-E P. aeruginosa DSer-Arg-DSer-Orn-c(Lys-Orn-Thr-Thr) 294
PyR P. aeruginosa DSer-Dab-Orn-DGln-Gln-DOrn-Gly 295
PyPaTII P. aeruginosa DSer-DOrn-Orn-Gly-DThr-Ser-cOrn 296
Py Pap P. aptata DAla-Lys-Thr-DSer-Orm-cOrn 297
Py Pau P. aureofaciens DSer-DOrn-Gly-DThr-Thr-Gln-Gly-DSer- 298
cDOrn
Ps P. fluorescens Lys-DAsp-Ala-DThr-Ala-cDOrn 299
Py I-III P. fluorescens Asn-DOrn-Lys-c(Thr-DAla-DAla-DOrn- 300
Lys)
Py Gm P. fluorescens DAla-Lys-Gly-Gly-Asp-DGln-DSer-Ala- 301
DAla-DAla-Ala-cOrn
Py Pf 12 P. fluorescens DSer-Lys-Gly-Orn-DSer-Ser-Gly-c(Lys- 302
DOrn-Glu-Ser)
Py Pf P. fluorescens c(DSer-Dab)-Gly-Ser-Asp-Ala-Gly-DAla- 303
2798 Gly-cOrn
Py Pf P. fluorescens Ser-Lys-Gly-Orn-c(Lys-DOrn-Ser) 304
13525
Py Pf P. fluorescens DAla-DLys-Gly-Gly-Asp-DGln-Dab-Ser- 305
17400 DAla-cOrn
Py 51W P. fluorescens DAla-DLys-Gly-Gly-DAsp-DGln-DSer-Ala- 306
Gly-DThr-cOrn
Py 9AW P. fluorescens DSer-Lys-His-DThr-Ser-cOrn 307
Ps A225 P. fluorescens DSer-DAla-DOrn-Gly-c(DSer-DAsp-DSer- 308
DThr)
Py Pf 1.3 P. fluorescens DAla-DLys-Gly-Gly-Asp-c(DGln-Dab)-Gly- 309
Ser-cOrn
Py Pf P. fluorescens DSer-Lys-Gly-Orn-Ser-DSer-Gly-c(Lys- 310
18.1 DOrn-Ser)
Py Pf P. fluorescens DSer-DOrn-Ala-Gly-DThr-Ala-cOrn 311
PL7
Py Pf P. fluorescens DLys-DOrn-Ala-Gly-DThr-Ser-cOrn 312
PL8
Py Pf P. fluorescens DSer-DSer-Orn-DSer-DSer-c(DSer-Orn- 313
BTP7 Lys-Lys)
Ps 589A P. putida Asp-Lys-Asp-DSer-Thr-DAla-DGlu-DSer- 314
cOrn
Py Pp 1,2 P. putida Ser-Thr-DSer-Orn-Asp-DGln-Dab-Ser- 315
DThr-cOrn
Py Pp P. putida Asp-DOrn-DDab-Thr-Gly-DSer-Ser-Asp- 316
C2,3 Thr
Py G4R P. putida Asp-Orn-DAsp-Dab-Gly-Ser-cOrn 317
Py P. putida Asp-DOrn-DDab-Thr-Gly-DSer-DSer-Thr- 318
PpBTP16 Asp
Py P. putida DSer-DAla-DOrn-Gly-DAla-DAsp-c(DSer- 319
Pp39167 DThr)
iPy Pp P. putida Asp-Ala-Asp-DOrn-Ser-cOrn 320
BTP1
Py P. tolaasii DSer-Lys-Ser-DSer-Thr-DSer-Orn-Thr- 321
PT2192 DSer-Orn
Ps 7SR1 Pseudomonas spp. DSer-DAsp-DThr-c(DSer-D-Orn-Ala-Gly- 322
DSer)
Ps A214 Pseudomonas spp. DSer-DAla-Gly-DSer-DAla-DAsp-DThr- 323
DOrn
Azoverdin Pseudomonas spp. Hse-DHse-Dab-DOrn-DSer-Orn 324
A. macrocytogenes
PF-S024 Corynebacteria SKRGRKRKDRRKKKANHGKRPNS 325
spp.
PF-001 S. epidermidis MNNWIIVAQLSVTVINEIIDIMKEKQKG 326
M. luteus GK
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
E. faecalis
C. jeikeium
PF-002 S. epidermidis NDDAQ 327
P. mirabilis
C. albicans
C. jeikeium
C. jejuni
PF-003 S. epidermidis MNNWIKVAQISVTVINEVIDIMKEKQN 328
M. luteus GGK
P. mirabilis
C. albicans
MRSA
C. jeikeium
PF-004 S. epidermidis ARLSKAIIIAVIVVYHLDVRGLF 329
B. subtilis
B. fragilis
E. coli
P. aeruginosa
C. albicans
S. pneumoniae
E. faecalis
C. jeikeium
PF-005 S. epidermidis MESIFKIKLMNGICRSENMNMKKKNKG 330
E. coli EKI
MRSA
S. pneumoniae
E. faecalis
PF-006 S. epidermidis MGIIAGIIKFIKGLIEKFTGK 331
M. luteus
E. coli
P. aeruginosa
MRSA
E. faecalis
C. jeikeium
C. jejuni
PF-007 S. epidermidis MGIIAGIIKVIKSLIEQFTGK 332
M. luteus
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-008 S. epidermidis MIEIGSIAYLNGGSKKYNHILNQENR 333
M. luteus
MRSA
C. jejuni
PF-009 M. luteus SKKYNHILNQENR 334
P. mirabilis
C. albicans
PF-010 S. epidermidis MDIDVNKLLQAFVYFKSFEKLRHNNS 335
M. luteus
E. coli
C. albicans
PF-011 M. luteus MFCYYKQHKGDNFSIEEVKNIIADNEM 336
E. coli KVN
P. aeruginosa
S. pneumoniae
C. jeikeium
PF-012 S. epidermidis WRGPNTEAGGKSANNIVQVGGAPT 337
M. luteus
P. mirabilis
E. coli
P. aeruginosa
MRSA
S. pneumoniae
C. jeikeium
C. jejuni
PF-013 M. luteus LIQKGLNQTFIVVIRLNNFIKKS 338
P. mirabilis
E. coli
P. aeruginosa
MRSA
S. pneumoniae
C. jeikeium
C. jejuni
PF-014 E. coli HPTDNKHN 339
C. jeikeium
PF-015 E. faecalis SIDKRNLYNLKYYE 340
C. jeikeium
PF-016 S. epidermidis RKQYDDLSFNFLY 341
E. faecalis
C. jeikeium
PF-017 E. coli ESIIE 342
PF-018 E. coli YYKTYFKEV 343
C. jeikeium
PF-020 S. epidermidis MKIILLLFLIFGFIVVVTLKSEHQLTLFSI 344
M. luteus
C. albicans
MRSA
S. pneumoniae
E. faecalis
PF-021 S. epidermidis FSLNFSKQKYVTVN 345
M. luteus
P. mirabilis
E. coli
C. albicans
E. faecalis
C. jeikeium
PF-022 M. luteus MINELKNKNSGIMNNYVVTKESKL 346
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-023 M. luteus MTKNTIISLENEKTQINDSENESSDLRKAK 347
C. jeikeium
PF-024 M. luteus DLRKAK 348
C. albicans
MRSA
E. faecalis
C. jeikeium
PF-025 S. epidermidis LLIIFRLWLELKWKNKK 349
M. luteus
P. mirabilis
E. coli
P. aeruginosa
MRSA
E. faecalis
C. jejuni
PF-026 S. epidermidis SIHFIN 350
M. luteus
P. mirabilis
C. albicans
MRSA
E. faecalis
C. jeikeium
PF-027 M. luteus HNARKYLEFISQKIDGDKLTKEDSL 351
MRSA
E. faecalis
C. jejuni
PF-028 S. epidermidis ALDCSEQSVILWYETILDKIVGVIK 352
M. luteus
MRSA
PF-029 S. epidermidis NSTNE 353
M. luteus
C. albicans
C. jejuni
PF-030 S. epidermidis MTCHQAPTTTHQSNMA 354
M. luteus
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-031 M. luteus MPHHSTTSSRIVVPAHQSNMASTPNLSI 355
C. albicans TP
PF-033 S. epidermidis MFIFKTTSKSHFHNNVKSLECIKIPINKNR 356
M. luteus
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
PF-034 M. luteus EPKKKHFPKMESASSEP 357
PF-035 S. epidermidis SFYESY 358
M. luteus
E. coli
C. albicans
MRSA
C. jeikeium
C. jejuni
PF-036 S. epidermidis ILNRLSRIVSNEVTSLIYSLK 359
M. luteus
P. mirabilis
E. coli
C. albicans
MRSA
S. pneumoniae
C. jejuni
PF-037 S. epidermidis MTKKRRYDTTEFGLAHSMTAKITLHQA 360
M. luteus LYK
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-038 M. luteus MAYKDEGKETKFAVKGYKD 361
PF-039 P. mirabilis MLEEKNKSL 362
C. jeikeium
PF-040 S. epidermidis MIHLTKQNTMEALHFIKQFYDMFFILNF 363
M. luteus NV
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-041 MRSA ELLVILPGFI 364
PF-042 S. epidermidis LLLSYFRYTGALLQSLF 365
M. luteus
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-043 M. luteus MIKNETAYQMNELLVIRSAYAK 366
C. jejuni
PF-044 S. epidermidis KLKKYIHKPD 367
M. luteus
MRSA
C. jeikeium
PF-045 S. epidermidis LDINDYRSTY 368
E. coli
E. faecalis
C. jejuni
PF-046 E. coli LDFYLTKHLTLML 369
E. faecalis
C. jeikeium
PF-047 S. mutans NQEPSLQQDKEQKDNKG 370
PF-048 S. epidermidis LYFAFKKYQERVNQAPNIEY 371
M. luteus
E. coli
MRSA
C. jeikeium
C. jejuni
PF-049 S. epidermidis AYYLKRREEKGK 372
MRSA
C. jeikeium
C. jejuni
PF-050 S. epidermidis SYYLKRREEKGK 373
M. luteus
E. coli
C. jeikeium
PF-051 S. epidermidis RFFNFEIKKSTKVDYVFAHVDLSDV 374
M. luteus
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
PF-052 S. epidermidis QELINEAVNLLVKSK 375
M. luteus
E. coli
MRSA
E. faecalis
C. jeikeium
C. jejuni
PF-053 S. epidermidis KLFGQWGPELGSIYILPALIGSIILIAIVTL 376
M. luteus ILRAMRK
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
PF-054 S. epidermidis VSISRFIGGGHVFNGNNKRNL 377
E. coli
PF-055 S. mutans GHVFNGNNKRNL 378
PF-056 S. epidermidis AEQLFGKQKQRGVDLFLNRLTIILSILFF 379
M. luteus VLMICISYLGM
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-057 S. epidermidis TMIVISIPRFEEYMKARHKKWM 380
M. luteus
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-058 S. epidermidis FADQSQDNA 381
M. luteus
E. coli
C. albicans
MRSA
C. jeikeium
C. jejuni
PF-060 E. coli HSSHL 382
C. albicans
C. jeikeium
PF-061 S. epidermidis GYNSYKAVQDVKTHSEEQRVTAKK 383
S. pneumoniae
PF-062 S. epidermidis MKKKRINNDILGRMIYSSSIDKRNLYNL 384
M. luteus KYYE
E. coli
P. aeruginosa
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-063 S. epidermidis IAAIIVLVLFQKGLLQIFNWILIQLQ 385
M. luteus
E. coli
P. aeruginosa
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-064 E. coli DYYGKE 386
PF-065 M. luteus LEKNTRDNYFIHAIDRIYINTSKGLFPES 387
E. coli ELVAWG
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
C. jeikeium
C. jejuni
PF-066 M. luteus IKGTVKAVDETTVVITVNGHGTELTFEK 388
E. coli PAIKQVDPS
C. jeikeium
PF-067 S. epidermidis DLIVKVHICFVVKTASGYCYLNKREAQ 389
M. luteus AAI
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-068 S. epidermidis SHLINNFGLSVINPSTPICLNFSPVFNLLT 390
M. luteus VYGITCN
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-069 E. faecalis FDPVPLKKDKSASKHSHKHNH 391
C. jejuni
PF-070 S. epidermidis SMVKSEIVDLLNGEDNDD 392
C. jejuni
PF-071 S. epidermidis HCVIGNVVDIANLLKRRAVYRDIADVIK 393
E. coli MR
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-073 S. epidermidis CPSVTMDACALLQKFDFCNNISHFRHFF 394
M. luteus AIKQPIER
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
PF-074 S. epidermidis RDIHPIYFMTKD 395
M. luteus
MRSA
PF-075 M. luteus FVNSLIMKDLSDNDMRFKYEYYNREKDT 396
E. coli
P. aeruginosa
MRSA
C. jeikeium
PF-076 S. epidermidis LYQYELLSKEEYLKCTLIINQRRNEQK 397
M. luteus
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-097 C. jeikeium QPTQGEQGTRPRRPTPMRGLLI 398
PF-099 S. epidermidis EIIAYLEGRFANA 399
M. luteus
E. coli
C. jeikeium
PF-101 S. mutans DPVPERQEQACACHRTAKPGK 400
PF-104 MRSA ERTAVNDLWI 401
C. jeikeium
PF-123 M. luteus TTRPQVAEDRQLDDALKETFPASDPISP 402
E. coli
PF-124 S. epidermidis MADGQIAAIAKLHGVPVATRNIRHFQSF 403
M. luteus GVELINPWSG
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
E. faecalis
C. jejuni
PF-125 S. epidermidis YVVGALVILAVAGLIYSMLRKA 404
M. luteus
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jejuni
PF-126 S. epidermidis FSPEAFGIGAAGVLGSFVTGLLIGWVAS 405
M. luteus LLRKAK
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-127 S. epidermidis MLRYLSLFAVGLATGYAWGWIDGLAA 406
M. luteus SLAV
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
PF-128 M. luteus GIKVVAARFEEIQFSENFDSIILA 407
P. aeruginosa
E. faecalis
PF-129 S. epidermidis MKLLARDPWVCAWNDIW 408
MRSA
E. faecalis
C. jeikeium
C. jejuni
PF-130 E. faecalis LQRSDEESMPRRHEKYS 409
C. jeikeium
C. jejuni
PF-131 S. epidermidis RRAAARTKGNRR 410
E. coli
MRSA
C. jeikeium
PF-132 S. epidermidis RPGDGAAEQGRSR 411
C. jeikeium
PF-133 S. epidermidis GDPTAGQKPVECP 412
C. jeikeium
C. jejuni
M. smegmatis
PF-134 S. epidermidis GKAMKRQDCSAL 413
C. jeikeium
PF-135 S. epidermidis PPARPARIPQTPTLHGASLFRQRS 414
M. luteus
E. coli
P. aeruginosa
MRSA
C. jeikeium
M. smegmatis
PF-136 S. epidermidis LRGRVGRITACGYPP 415
M. luteus
P. mirabilis
E. coli
MRSA
E. faecalis
C. jeikeium
C. jejuni
M. smegmatis
PF-137 S. epidermidis VLGKGHDLLDVGKTALKSRVFAWLGGS 416
P. mirabilis
S. pneumoniae
C. jeikeium
C. jejuni
PF-138 S. epidermidis AVHHSLLFR 417
M. luteus
P. mirabilis
E. coli
C. albicans
MRSA
C. jeikeium
C. jejuni
PF-139 S. epidermidis ALSKPAIQARTLCRRQDPP 418
M. luteus
P. mirabilis
E. coli
P. aeruginosa
C. albicans
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-140 S. epidermidis FHRRVIRASEWALTTRSFSTPLRSAAR 419
M. luteus
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
M. smegmatis
PF-141 S. epidermidis VVRRFQGM 420
M. luteus
C. albicans
MRSA
C. jeikeium
PF-142 S. mutans GIDRGCQAAR 421
PF-143 S. epidermidis LSPRPIIVSRRSRADNNNDWSR 422
MRSA
C. jeikeium
PF-144 S. epidermidis RSGQPVGRPSRRAWLR 423
M. luteus
E. coli
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-145 S. epidermidis GIVLTGRAGLVSGACSMALGVGLG 424
M. luteus
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
M. smegmatis
PF-146 S. epidermidis GCGKRRIITKSASRDTR 425
M. luteus
P. aeruginosa
C. albicans
MRSA
C. jeikeium
PF-147 S. epidermidis RRPRRRRSGHGQSASAA 426
M. luteus
MRSA
PF-148 S. epidermidis RRGCTERLRRMARRNAWDLYAEHFY 427
M. luteus
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
M. smegmatis
PF-149 S. epidermidis GKVSVLTRVPRSLGGAPANQ 428
M. luteus
E. coli
MRSA
C. jeikeium
PF-150 S. epidermidis EIQAKGTG 429
MRSA
PF-151 S. epidermidis EEYPARVPLSGEDVTEARRH 430
MRSA
E. faecalis
C. jeikeium
PF-152 S. epidermidis VGYFIWKDSHSRKG 431
C. albicans
MRSA
E. faecalis
C. jeikeium
PF-153 M. luteus GILARADCSQIA 432
P. mirabilis
E. coli
MRSA
PF-154 S. mutans GIKKSKHPSTDDYVVKTTIDSL 433
PF-155 C. jeikeium GRYGDDSKERQGRAQ 434
PF-156 S. epidermidis LITAEQPATAPIAGK 435
C. jeikeium
PF-157 S. epidermidis HTAVVWLAGVSGCVALSHCEPA 436
M. luteus
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-158 S. epidermidis VRLESRPADLPE 437
PF-159 S. epidermidis TMAFVEKAQLRVPVGDDLPV 438
PF-160 S. epidermidis SFHASLTKNEKPIKSTG 439
PF-161 S. epidermidis RGRALASTATTRPARRRR 440
M. luteus
E. coli
C. jejuni
PF-162 S. epidermidis GIRRLHSVENLNREISHRMAGLR 441
MRSA
PF-163 S. epidermidis TSWLRAAERQEIGEPTKTFGEKTTSL 442
PF-164 S. epidermidis EEVSRALAGIGLGLGCRIG 443
M. luteus
E. coli
C. jeikeium
PF-165 MRSA GPVSVVASLRRGTTVQRHSQNNHNKG 444
C. jejuni KP
PF-166 E. coli SKAVSRKRSI 445
C. jeikeium
PF-167 S. epidermidis AIEGVIKKGACFKLLRHEMF 446
E. coli
C. albicans
MRSA
C. jeikeium
C. jejuni
PF-168 S. epidermidis VLPFPAIPLSRRRACVAAPRPRSRQRAS 447
M. luteus
E. coli
C. albicans
MRSA
C. jeikeium
C. jejuni
PF-169 S. epidermidis APGSAADSPRSRADD 448
E. coli
C. albicans
E. faecalis
C. jeikeium
PF-170 S. epidermidis RLARGRPTNLCGRRG 449
M. luteus
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jejuni
PF-171 S. epidermidis TQVTLCRTW 450
E. coli
P. aeruginosa
S. pneumoniae
PF-172 S. epidermidis LTGVRRPWRAPWAGTSGWALR 451
M. luteus
E. coli
P. aeruginosa
MRSA
E. faecalis
C. jejuni
PF-173 S. epidermidis AGRTAIVQGGG 452
M. luteus
P. mirabilis
E. coli
P. aeruginosa
C. albicans
C. jeikeium
C. jejuni
PF-174 S. epidermidis RGGDSPARRRPGLAGPGGPG 453
P. aeruginosa
C. jeikeium
PF-175 S. epidermidis RRRPAGQRPEKASQAMIAA 454
E. faecalis
PF-176 S. epidermidis RLTSNQFLTRITPFVFAQH 455
M. luteus
P. mirabilis
E. coli
C. albicans
MRSA
E. faecalis
C. jeikeium
PF-177 M. luteus VTSEPGIAHDIRLLPRAAAFR 456
MRSA
E. faecalis
C. jeikeium
PF-178 S. epidermidis EVYSSPTNNVAITVQNN 457
M. luteus
B. subtilis
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-180 S. epidermidis SGLGDLGFSSEAK 458
M. luteus
P. aeruginosa
C. albicans
MRSA
E. faecalis
C. jejuni
M. smegmatis
PF-181 S. epidermidis GIAPRRNEWGAVGGR 459
M. luteus
E. coli
MRSA
E. faecalis
C. jeikeium
PF-182 S. epidermidis LPATRDKTRVPASVAGAP 460
M. luteus
E. coli
E. faecalis
C. jeikeium
PF-183 S. epidermidis KPGISVENRQ 461
M. luteus
E. coli
C. albicans
MRSA
E. faecalis
C. jeikeium
PF-184 S. epidermidis LIADRHIRA 462
M. luteus
E. coli
P. aeruginosa
C. albicans
MRSA
C. jeikeium
PF-185 E. coli RPAQARQGPGGLIADRHIRA 463
P. aeruginosa
PF-186 S. epidermidis DADKNLSLERDRFAWRVAAP 464
M. luteus
E. coli
P. aeruginosa
MRSA
C. jeikeium
PF-187 S. epidermidis EIQKIAKGVSGQVYGPSRQITISKKR 465
M. luteus
E. coli
MRSA
PF-188 S. epidermidis ARTFAGRLGTRYFGGLMRSTKA 466
M. luteus
E. coli
C. albicans
MRSA
E. faecalis
PF-189 S. epidermidis GNLTRSREAARATQ 467
M. luteus
C. albicans
MRSA
E. faecalis
C. jejuni
PF-190 S. epidermidis HFILRKPLLFMIHSLKTGPLDRF 468
M. luteus
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-191 E. coli QFCNFAWLFLASNNAQVSALA 469
P. aeruginosa
C. jejuni
PF-192 S. epidermidis VEEDEAPPPHY 470
M. luteus
P. aeruginosa
C. albicans
E. faecalis
C. jeikeium
PF-193 S. epidermidis PPHCPPGHAKKGWC 471
M. luteus
E. coli
MRSA
E. faecalis
C. jejuni
PF-194 C. jeikeium MKGNKLATAHEQPVKNSAPPL 472
PF-195 S. epidermidis EMAEGSADDRLRKTPRDC 473
M. luteus
E. faecalis
C. jeikeium
PF-196 S. epidermidis TTARYIRRQCHTSITPLSQG 474
M. luteus
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jejuni
PF-197 S. epidermidis CNALLRRGHPPSAL 475
M. luteus
C. albicans
E. faecalis
C. jejuni
PF-200 S. epidermidis GIELKSLIMAQIERWRQA 476
M. luteus
MRSA
E. faecalis
C. jeikeium
PF-201 S. epidermidis GCRPASLSDADPDGR 477
M. luteus
E. coli
C. albicans
E. faecalis
C. jeikeium
C. jejuni
PF-202 S. epidermidis ALNRASLRLALGE 478
M. luteus
E. coli
MRSA
E. faecalis
C. jeikeium
C. jejuni
PF-203 S. epidermidis SWKCHHLAI 479
M. luteus
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jejuni
PF-204 S. epidermidis ALQKQDMNLPSVKNQLVFLKSTG 480
P. mirabilis
E. coli
P. aeruginosa
C. albicans
C. jejuni
PF-205 S. epidermidis AGVLETPRCRGEYGAN 481
M. luteus
E. coli
P. aeruginosa
C. albicans
MRSA
E. faecalis
C. jeikeium
C. jejuni
PF-206 M. luteus KLRSASKKSLQEKSCGIMPEKPAG 482
C. albicans
C. jeikeium
C. jejuni
PF-207 M. luteus AAGCRDLGSLSSLVTNPS 483
C. jeikeium
PF-208 S. epidermidis DAYHCHLVRSPDAHDLSMRIGFV 484
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-209 C. albicans NYAVVSHT 485
C. jeikeium
C. jejuni
PF-210 S. epidermidis EREDGCDAMPLP 486
P. aeruginosa
C. albicans
MRSA
E. faecalis
C. jeikeium
C. jejuni
PF-211 S. epidermidis DSFDSLSPFRERGGEREDGCDAMPLP 487
M. luteus
E. coli
P. aeruginosa
C. albicans
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
M. smegmatis
PF-212 M. luteus NDSKASN 488
P. aeruginosa
PF-213 S. epidermidis MTTGVDFIIEKV 489
PF-214 S. mutans GHLRVCWVFSASLLTPFRSATLI 490
S. epidermidis
M. luteus
E. coli
P. aeruginosa
A. baumannii
PF-215 S. epidermidis ELKITNYNVNTVLYRYYKWGNDLCE 491
M. luteus
P. aeruginosa
A. baumannii
PF-216 S. mutans ESVDKITEALEEDGFPAKVQ 492
E. coli
PF-217 S. mutans DWEFTHKTIPQKK 493
PF-218 S. epidermidis SETPEKPVGTFFYSIYYKIIL 494
M. luteus
P. aeruginosa
A. baumannii
PF-219 S. epidermidis FLALAVIAGLFKVILIYAAPYLK 495
M. luteus
P. aeruginosa
A. baumannii
PF-221 S. epidermidis VFDNIDINF 496
M. luteus
P. aeruginosa
PF-222 S. epidermidis HIKETR 497
PF-223 S. epidermidis VKFCIECQTKLERKRR 498
M. luteus
A. baumannii
PF-224 S. epidermidis DYFYITLSQKNTF 499
P. aeruginosa
A. baumannii
PF-225 S. epidermidis MNCASPEFKKLMELYK 500
PF-226 A. baumannii LMFFSENMDKRDTLSGKFRYFAGSKVI 501
KLMNWLSENGK
PF-228 S. mutans NQLGSQAFAQL 502
PF-229 S. epidermidis DPILIQIGFTRFALRKAEAEKIEIQVEEGV 503
M. luteus PA
P. aeruginosa
A. baumannii
PF-230 S. mutans EDKPTNTIQEIKPVKWQ 504
PF-231 S. mutans AVRDFKKSVREEDEAASLNSPRTIDAQ 505
VKTSESTSVKS
PF-232 S. epidermidis FDQLYALEREGKLDELLA 506
M. luteus
PF-233 S. epidermidis DANAMARTTIAIVYILALIALTISYSL 507
M. luteus
P. aeruginosa
A. baumannii
PF-234 S. epidermidis RTPYILRS 508
M. luteus
PF-235 S. epidermidis GIPFSKPHKRQVNYMKSDVLAYIEQNK 509
M. luteus MAHTA
PF-236 S. mutans KEIRTATVAELNAKRRLTSAEQALAEVS 510
S. epidermidis
E. coli
C. albicans
S. pneumoniae
E. faecalis
PF-237 S. epidermidis YVKPKVGVHE 511
PF-238 S. mutans RNAVVVTEATFPKYEEEITNYLNRRFGE 512
S. epidermidis DWSLKLEKCSVA
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
PF-239 S. mutans PKHNVVTGVSVDLDYKP 513
E. coli
PF-240 S. mutans RITEVPPDEHSDR 514
E. coli
PF-242 S. mutans KLFEDPLIKSKAVENFQTTWHEQCLAK 515
E. coli ELAKNM
PF-244 S. epidermidis HMRTISYLLAFAKFSLFIPPKQSLKRL 516
M. luteus
P. aeruginosa
A. baumannii
PF-245 S. epidermidis MNDVKPVVQPKQTLKAFLVQLLSVRA 517
M. luteus GVYIKQNNQLPKTKG
P. aeruginosa
A. baumannii
PF-246 S. mutans QPDEKAEFFDPSLDKVYRHPTFYHIPDG 518
IEHM
PF-247 S. epidermidis ETAASETH 519
PF-248 S. mutans ILSKLWFWMINSLGVVLLVSYWLLAK 520
S. epidermidis WGVA
M. luteus
E. coli
P. aeruginosa
A. baumannii
PF-249 S. epidermidis INSRYKISF 521
M. luteus
PF-252 S. mutans MKKLVAALAVIVILTGCVYDPVNYDKI 522
HDQEFQDHLRQNG
PF-253 S. epidermidis VRDDDS 523
M. luteus
PF-254 S. epidermidis FIYGVGFVPHFWLWKWLFSPWIAWPL 524
M. luteus MLLGYYIWFLT
P. aeruginosa
A. baumannii
PF-255 P. aeruginosa DHKINESQHNPFRSDSNKQNVDFF 525
PF-256 S. epidermidis EYFKQVYVKNEKIYSFWICKDLSPKEA 526
AKRAEDILVKLK
PF-257 S. epidermidis VWENRKKYLENEIERHNVFLKLGQEVI 527
KGLNALASRGR
PF-259 S. epidermidis LPFSKIGRRVSYKKKDVLKYEQSKTVL 528
P. aeruginosa NTAQLATV
A. baumannii
PF-262 S. mutans DPHSEIDVTRYCQLHHFTCQTMQISERE 529
S. epidermidis FHYLIETQ
M. luteus
E. coli
P. aeruginosa
A. baumannii
PF-263 S. epidermidis NLKKCPC 530
M. luteus
A. baumannii
PF-265 S. epidermidis MKTLFFPLFLIIFVLIIQALDQSYQKKIGI 531
M. luteus SKPQKHPEFMQ
A. baumannii
PF-266 S. mutans DQEKKNKTEESTEQ 532
PF-267 M. luteus SDDKRTD 533
PF-268 S. mutans EVLLSDLRPDIFSET 534
PF-270 S. epidermidis MYLTPYAWIAVGSIFAFSVTTIKIGDQN 535
M. luteus DEKQKSHKNDVHKR
P. aeruginosa
PF-271 S. epidermidis AAQPQTTSP 536
M. luteus
P. aeruginosa
A. baumannii
PF-273 S. epidermidis LVGALLIFVALIYMVLKGNADKN 537
M. luteus
P. aeruginosa
A. baumannii
PF-275 S. mutans LVSGVANTVKNTAHTVGNTAKHAGHV 538
AADTTVKATKKQQVK
PF-276 S. epidermidis LDLALSTNSLNLEGFSF 539
PF-278 M. luteus LSLATFAKIFMTRSNWSLKRFNRL 540
A. baumannii
PF-279 S. mutans SHIGFISISACLAVLLGIARLFVWTWVKF 541
S. epidermidis FA
M. luteus
E. coli
P. aeruginosa
A. baumannii
PF-281 S. mutans SYNTYYNKLIHGQRTPDGM 542
E. coli
PF-282 S. mutans QNNDTSAWCGSAHKNGNS 543
PF-283 B. subtilis MIRIRSPTKKKLNRNSISDWKSNTSGRF 544
B. fragilis FY
C. difficile
PF-284 C. difficile MRYITYSLIPRLLSKKVIHQQ 545
PF-285 S. mutans VPAKLLRVIDEIPE 546
PF-288 S. mutans IYQLLNIEYSEDD 547
E. coli
PF-289 C. difficile MGRHLWNPSYFVATVSENTEEQIRKYR 548
KNK
PF-291 S. mutans DVDGAIESEL 549
E. coli
PF-292 S. epidermidis SFVSTTVRLIFEESKRYKF 550
B. subtilis
B. fragilis
PF-294 S. epidermidis DFLVNFLWFKGELNWGKKRYK 551
C. difficile
PF-295 C. difficile NIQVYESECGNYIFKKSDESFLIDIFDKN 552
GTH
PF-297 S. epidermidis ISKGIDDIVYVINKILSIGNIFKIIKRK 553
B. subtilis
B. fragilis
PF-299 B. subtilis LATKLKYEKEHKKM 554
PF-300 B. subtilis VKDVLLELFNKIIGA 555
C. difficile
PF-301 C. difficile GIVLIGLKLIPLLANVLN 556
PF-304 S. mutans LVKDTSDIKNDLNNIEIVTSKNSNDIAKL 557
KSVK
PF-305 C. difficile MREWICPSCNETHDRDINASINILKEGL 558
RLITIQNK
PF-306 C. difficile GCILPHKKDNYNYIMSKFQDLVKITSKK 559
PF-307 S. epidermidis MKRRRCNWCGKLFYLEEKSKEAYCCK 560
B. subtilis ECRKKAKKVKK
B. fragilis
C. difficile
PF-308 C. difficile QQYLILDRM 561
PF-309 S. mutans GIPGMTAAPAEENEQEENADEE 562
E. coli
PF-311 C. difficile IDAVTKKKTTCMIRAPTKIPIAHTDN 563
PF-313 S. epidermidis YITSHKNARAIIKKFERDEILEEVITHYL 564
C. difficile NRK
PF-314 S. mutans ECLKKAIKSKALNKAFKIDVPDEVYDN 565
LLMELEEYEK
PF-317 S. mutans LILVSDI 566
PF-319 S. epidermidis SIGSMIGMYSFRHKTKHIKFTFGIPFILFL 567
B. subtilis QFLLVYFYILK
C. difficile
PF-320 S. mutans DSGYYALLENKEERVVWDGEVVANNI 568
E. coli FNNLWIVVNKVKTG
PF-323 S. mutans ARESIEKSHVPVDATIVGVVDSFEVFDE 569
PF-324 C. difficile HFSLL 570
PF-325 S. mutans LTIDEKLRNHR 571
E. coli
PF-326 S. mutans VIVGNLGAQKEKRNDTPISAKKDIMGD 572
E. coli KTVRVRADLHH
PF-328 S. mutans NGNEKAFSEVENLVK 573
PF-329 S. epidermidis IGILFDKSVRKY 574
PF-333 S. mutans YMTKKLVEMAEQQMAGKSNR 575
PF-334 S. epidermidis QQYLILDRM 576
C. difficile
PF-336 S. mutans MLTSRKKRLKKIVEEQNKKDESI 577
E. coli
PF-337 S. epidermidis YMTKKLVEMAERQMAGK 578
PF-338 S. mutans KGTSCPDQLSKAIRQSI 579
PF-340 S. mutans VKDVLLELFNKIIGA 580
E. coli
PF-344 B. subtilis DERLPEAKAIRNFNGSVMVLGR 581
C. jejuni
PF-347 S. epidermidis GIFTGVTVVVSLKHC 582
B. subtilis
B. fragilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
PF-348 B. subtilis ESASAAEWYNPNMNVKKAICMG 583
E. coli
P. aeruginosa
C. albicans
E. faecalis
C. jejuni
PF-349 S. epidermidis MPKSCHVPVLCDFFFLVIIKFLALFKTIQS 584
B. subtilis
B. fragilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-350 S. epidermidis LAVILRAIVY 585
E. coli
E. faecalis
C. jeikeium
C. jejuni
PF-351 S. mutans YLFFKGKKVAEEEATKDEVKR 586
PF-352 C. jeikeium RVKKIG 587
PF-353 S. epidermidis EKTNFKGVKRNFYKKASFFV 588
M. luteus
B. subtilis
E. coli
C. albicans
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-354 S. epidermidis FTFSKCRASNGRGFGTLWL 589
B. subtilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-355 S. epidermidis WIAIGLLLYFSLKNQ 590
B. subtilis
B. fragilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-356 S. epidermidis VSIKIGAIVIGMIGLMELLTE 591
B. subtilis
B. fragilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-357 S. epidermidis MLTIIIGFIFWTMTLMLGYLIGEREGRK 592
M. luteus HE
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-358 S. epidermidis RNTAHNIKWRSKN 593
B. subtilis
E. coli
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-359 S. epidermidis MTVMEDPGSEQRNKIQSPMKGEDFSAL 594
B. fragilis FGR
P. aeruginosa
C. albicans
MRSA
E. faecalis
C. jeikeium
PF-360 S. epidermidis MEQKVKVIFVPRSKPDNQLKTFVSAVL 595
B. subtilis FKA
E. coli
P. aeruginosa
C. albicans
E. faecalis
C. jeikeium
C. jejuni
PF-361 S. epidermidis NQVTEGIRLLVE 596
E. coli
E. faecalis
C. jejuni
PF-362 S. epidermidis NIERILKEKVWMIRCVE 597
E. coli
P. aeruginosa
C. albicans
E. faecalis
C. jejuni
PF-363 B. subtilis SMLSVTVMCLMHASVAANQAMEKKV 598
E. coli
P. aeruginosa
C. albicans
S. pneumoniae
E. faecalis
PF-364 S. epidermidis LVNGIKI 599
B. fragilis
P. aeruginosa
C. jeikeium
C. jejuni
PF-365 S. epidermidis LYKQKIQLEEELEKLKDDRQ 600
B. subtilis
B. fragilis
P. aeruginosa
C. albicans
PF-366 S. epidermidis ALCSVIKAIELGIINVHLQ 601
M. luteus
B. fragilis
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-367 B. subtilis TKTPGTFTPGTGIQKTAVPL 602
PF-368 C. jeikeium MLKQTA 603
C. jejuni
PF-369 B. subtilis MSEAVNLLRGARYSQRYAKNQVPYEVI 604
B. fragilis IEK
E. coli
P. aeruginosa
C. albicans
S. pneumoniae
C. jeikeium
C. jejuni
PF-370 S. epidermidis VIFLHKESGNLKEIFY 605
E. coli
P. aeruginosa
E. faecalis
C. jejuni
PF-371 S. epidermidis TFIYNEF 606
B. fragilis
C. jejuni
PF-372 C. jeikeium KKQDKRIEDKYKRMKKGD 607
C. jejuni
PF-373 S. epidermidis HFYLLFER 608
E. coli
P. aeruginosa
C. albicans
MRSA
E. faecalis
C. jejuni
PF-374 S. epidermidis HLFFVKGMFILCQKNQINDE 609
B. subtilis
B. fragilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-375 S. epidermidis MDSAKAQTMRTDWLAVSCLVASAYLR 610
B. subtilis SMLA
B. fragilis
E. coli
P. aeruginosa
C. albicans
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-376 S. epidermidis MTVFEALMLAIAFATLIVKISNKNDKK 611
B. subtilis
B. fragilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-378 B. subtilis ESAKSNLNFLMQEEWALFLLL 612
B. fragilis
E. coli
P. aeruginosa
C. jeikeium
PF-379 S. epidermidis VFVVLFIIYLASKLLTKLFPIKK 613
B. subtilis
B. fragilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-380 S. epidermidis KKIIPLITLFVVTLVG 614
B. subtilis
B. fragilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-381 E. coli QGANPCQQVGFTVNDPDCRLAKTV 615
P. aeruginosa
C. jejuni
PF-382 S. epidermidis KYKCSWCKRVYTLRKDHKTAR 616
B. subtilis
B. fragilis
E. coli
P. aeruginosa
E. faecalis
C. jeikeium
C. jejuni
PF-383 S. epidermidis WSEIEINTKQSN 617
B. subtilis
B. fragilis
E. coli
C. jejuni
PF-384 E. faecalis HISKERFEAY 618
C. jeikeium
C. jejuni
PF-385 S. epidermidis MIKKSILKIKYYVPVLISLTLILSA 619
E. coli
P. aeruginosa
C. albicans
E. faecalis
PF-386 S. epidermidis FTLTLITTIVAILNYKDKKK 620
B. subtilis
B. fragilis
E. coli
P. aeruginosa
C. albicans
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-387 B. subtilis GAVGIAFFAGNMKQDKRIADRQNKKSE 621
E. coli KK
P. aeruginosa
E. faecalis
C. jeikeium
C. jejuni
PF-388 E. faecalis ITPLLDEIGKVCIDKISK 622
C. jeikeium
C. jejuni
PF-389 S. epidermidis GLQFKEIAEEFHITTTALQQWHKDNGY 623
C. albicans PIYNKNNRK
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-390 S. epidermidis VVAYVITQVGAIRF 624
P. aeruginosa
C. albicans
MRSA
PF-392 S. epidermidis DPAGCNDIVRKYCK 625
B. subtilis
S. pneumoniae
C. jeikeium
C. jejuni
PF-393 S. epidermidis DLVQSILSEFKKSG 626
E. coli
C. albicans
MRSA
S. pneumoniae
C. jejuni
PF-394 S. epidermidis VLKEECYQKN 627
MRSA
C. jejuni
PF-395 S. epidermidis YCVPLGNMGNMNNKIW 628
E. coli
P. aeruginosa
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-396 S. epidermidis LIYTILASLGVLTVLQAILGREPKAVKA 629
E. coli
P. aeruginosa
C. albicans
E. faecalis
C. jeikeium
PF-397 S. epidermidis VEDLMEDLNA 630
MRSA
S. pneumoniae
E. faecalis
C. jejuni
PF-398 S. epidermidis ILVVLAGILLVVLSYVGISKFKMNC 631
B. subtilis
B. fragilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-399 S. epidermidis FPIISALLGAIICIAIYSFIVNRKA 632
M. luteus
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jejuni
PF-400 S. epidermidis VIAWKFRNKFENSGV 633
E. coli
S. pneumoniae
E. faecalis
C. jeikeium
PF-401 S. epidermidis YWLSRVTTGHSFAFEKPVPLSLTIK 634
E. coli
P. aeruginosa
MRSA
E. faecalis
C. jejuni
PF-402 S. epidermidis FIDVLKSKINEFLN 635
P. aeruginosa
E. faecalis
C. jejuni
PF-403 E. coli LLSTEQLLKYYDGETFDGFQLPSNE 636
P. aeruginosa
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-404 S. epidermidis VLYFQATVV 637
E. coli
P. aeruginosa
E. faecalis
C. jeikeium
C. jejuni
PF-405 S. epidermidis LVRIEVDDLEEWYERNFI 638
E. coli
E. faecalis
PF-406 E. coli YLEMNADYLSNMDIFDELWEKYLENNK 639
C. jejuni
PF-407 S. epidermidis KPKNKKEKTVISYEKLLSMY 640
B. subtilis
E. coli
P. aeruginosa
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-408 S. epidermidis YCVPLGNMGNMNNKIW 641
E. coli
P. aeruginosa
MRSA
E. faecalis
C. jeikeium
C. jejuni
PF-409 S. epidermidis DLVQSILSEFKKSG 642
MRSA
C. jeikeium
C. jejuni
PF-410 S. epidermidis FALELIALCRNLFIVYFP 643
M. luteus
B. fragilis
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
PF-411 M. luteus WVAVAILLNIALQTQLT 644
B. subtilis
B. fragilis
P. mirabilis
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-412 M. luteus TSGWLGQLEQ 645
E. coli
C. albicans
C. jeikeium
C. jejuni
PF-413 P. aeruginosa TFAGSIKIGVPDLVHVTFNCKR 646
C. albicans
C. jejuni
PF-414 E. coli LLNKKLE 647
C. albicans
C. jeikeium
PF-416 S. pneumoniae SKAGLYGKIERSDKRE 648
C. jeikeium
PF-417 S. epidermidis DSYFRS 649
C. jeikeium
C. jejuni
PF-418 S. epidermidis FFLVHFYIRKRKGKVSIFLNYF 650
M. luteus
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-421 C. jeikeium KHCFEITDKTDVV 651
PF-422 C. albicans MSRKKYENDEKSQKKLKIGRKSDVFYG 652
MRSA IID
C. jeikeium
PF-423 S. epidermidis AGKKERLLSFREQFLNKNKKK 653
M. luteus
E. coli
S. pneumoniae
E. faecalis
C. jeikeium
PF-424 S. epidermidis IAAFVTSRAFSDTVSPI 654
C. albicans
MRSA
PF-425 S. epidermidis MMELVLKTIIGPIVVGVVLRIVDKWLN 655
M. luteus KDK
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
C. jeikeium
PF-426 S. epidermidis MLQKYTQMISVTKCIITKNKKTQENVD 656
E. coli AYN
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-427 M. luteus YVLEYHGLRATQDVDAFMAL 657
P. aeruginosa
C. albicans
C. jejuni
PF-428 S. epidermidis ENEESIF 658
C. albicans
E. faecalis
C. jeikeium
PF-429 S. epidermidis AATLICVGSGIMSSL 659
S. pneumoniae
C. jeikeium
PF-430 S. epidermidis AVVCGYLAYTATS 660
M. luteus
E. coli
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-431 S. epidermidis VAYAAICWW 661
M. luteus
E. coli
P. aeruginosa
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-432 S. epidermidis FNGDSEFFLCIAF 662
M. luteus
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-433 S. epidermidis MRKEFHNVLSSGQLLADKRPARDYNRK 663
E. coli
S. pneumoniae
C. jeikeium
PF-434 S. epidermidis GQLLADKRPARDYNRK 664
M. luteus
S. pneumoniae
C. jeikeium
PF-435 C. jeikeium MSRWDGHSDKGEAPAGKPPMHGFGLN 665
GENK
PF-436 C. jeikeium KKHVLVGKQEKNG 666
PF-438 S. epidermidis QPYFQNQFKKITGYTPLQYRKEKR 667
E. coli
S. pneumoniae
C. jeikeium
C. jejuni
PF-439 S. epidermidis RVLVLKKFHGIMDGNRNVAVFFVGQ 668
M. luteus
B. fragilis
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-440 S. epidermidis MFIISPDLFNIAVILYILFFIHDILLLILS 669
M. luteus
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-441 C. jeikeium TQVHKMARGIDPGPANGIYR 670
PF-442 S. epidermidis MQIFYIKTKIFLSFFLFLLIFSQCFYKIEE 671
E. coli
C. albicans
S. pneumoniae
E. faecalis
PF-443 S. epidermidis KLLYFFNYFENLQQVHLLVQL 672
M. luteus
P. mirabilis
E. coli
P. aeruginosa
C. albicans
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-444 M. luteus MAAKLWEEGKMVYASSASMTKRLKL 673
C. albicans AMSKV
S. pneumoniae
C. jeikeium
PF-445 M. luteus ASMTKRLKLAMSKV 674
S. pneumoniae
C. jeikeium
PF-446 M. luteus SGNEKV 675
C. jeikeium
PF-447 S. epidermidis IDKSRNKDQFSHIFGLYNICSG 676
M. luteus
E. coli
S. pneumoniae
PF-448 S. epidermidis SLQSQLGPCLHDQRH 677
M. luteus
P. mirabilis
E. coli
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-450 S. epidermidis HRNLIILQRTIFI 678
M. luteus
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-451 S. epidermidis MVNYIIGSYMLYREQNNNEALRKFDIT 679
M. luteus LAM
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
M. smegmatis
PF-452 M. luteus MNNWIKVAQISVTVINEVIDIMKEKQN 680
P. aeruginosa GGK
C. albicans
S. pneumoniae
E. faecalis
C. jeikeium
M. smegmatis
PF-453 M. luteus IIQDIAHAFGY 681
E. coli
P. aeruginosa
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-454 S. epidermidis MSVFVPVTNIFMFIMSPIFNVNLLHFKV 682
M. luteus YI
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
M. smegmatis
PF-456 C. albicans TCVKPRTIN 683
MRSA
E. faecalis
C. jeikeium
C. jejuni
PF-457 C. albicans INKYHHIA 684
S. pneumoniae
E. faecalis
C. jeikeium
PF-458 S. epidermidis ISLIIFIMLFVVALFKCITNYKHQS 685
M. luteus
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-459 P. aeruginosa EKRMSFNENQSHRPLL 686
PF-460 S. epidermidis MEHVLPFQNTPPNIVIIYKDFTHLKSITFS 687
M. luteus
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
M. smegmatis
PF-461 E. coli MTLAIKNCSVTKCLGFGDFVNDDSDSY 688
S. pneumoniae FDA
PF-462 E. faecalis KNKTDTL 689
C. jeikeium
PF-463 S. epidermidis MVILVFSLIFIFTDNYLVYQSKSIKEDVMI 690
E. coli
P. aeruginosa
C. albicans
S. pneumoniae
E. faecalis
M. smegmatis
PF-464 S. epidermidis VDMVNRFLGN 691
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-465 S. epidermidis KPVGKALEEIADGKIEPVVPKEYLG 692
M. luteus
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-466 MRSA VRKSDQ 693
C. jeikeium
C. jejuni
PF-467 MRSA YYKDYFKEI 694
E. faecalis
C. jeikeium
C. jejuni
PF-469 S. epidermidis YKVNYNNIDNHFNTLRH 695
M. luteus
P. mirabilis
E. coli
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-470 M. luteus PYSDSYATRPHWEQHRAR 696
E. coli
MRSA
E. faecalis
C. jeikeium
C. jejuni
PF-471 S. epidermidis MVGKIRGVTPRNDLLNANITGQLNLNY 697
M. luteus RLI
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-472 S. epidermidis MHISHLLDEVEQTEREKAVNVLENMNG 698
E. coli NVI
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-473 S. epidermidis MAADIISTIGDLVKWIIDTVNKFKK 699
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
PF-474 S. epidermidis MHRNLVLVKMEPIPHIMIIANQIGIIIEKA 700
M. luteus
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
M. smegmatis
PF-475 S. epidermidis MREKVRFTQAFKLFWTNYFNFKGRSRR 701
M. luteus SEY
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-476 M. luteus WADAQYKLCENCSE 702
P. mirabilis
C. albicans
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-477 S. epidermidis HKNKLNIPHIKS 703
M. luteus
C. albicans
S. pneumoniae
C. jeikeium
C. jejuni
PF-478 S. epidermidis HLFILKSHLKPFPPFRYTYD 704
M. luteus
P. mirabilis
E. coli
C. albicans
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-479 S. epidermidis AYILKRREEKNK 705
M. luteus
P. mirabilis
E. coli
C. albicans
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-480 S. epidermidis MVEILVNTAISVYIVALYTQWLSTRDNL 706
M. luteus KA
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
M. smegmatis
PF-481 C. jeikeium DELYEIMDKVIEEFNKDIEQNNNNGNN 707
EDLTENKIN
PF-482 S. epidermidis LVGYVRTSGTVRSYKIN 708
M. luteus
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-483 P. mirabilis EDNKDKKDKKDK 709
C. jeikeium
C. jejuni
PF-484 S. epidermidis HKKDIRKQVFKN 710
M. luteus
P. mirabilis
E. coli
E. faecalis
C. jeikeium
C. jejuni
PF-486 S. mutans MQKEGEEDY 711
PF-487 S. mutans MYKAIAVLAMTIMAFFIFVYPFFIVGLILG 712
E. coli
PF-488 S. mutans YPNEQGHHKNNLKNIIIE 713
E. coli
PF-489 S. mutans KVDRVSTTITEKIK 714
PF-490 S. mutans RLILVSGNATVQK 715
E. coli
PF-491 S. mutans IHQYSSKPDIVGQEAKTVQQINS 716
E. coli
PF-492 S. mutans IQIDAASFYSISKSTIK 717
B. subtilis
E. coli
PF-493 S. mutans PGAFFFCRGRGCWCGIGW 718
B. subtilis
E. coli
PF-494 S. mutans FTEPLRPLQAKGQIISIKPSTSSS 719
PF-495 S. mutans KGIYKKRTY 720
E. coli
PF-496 S. mutans EVTKRLVALAQQQLRG 721
E. coli
PF-497 S. mutans LVLRICTDLFTFIKWTIKQRKS 722
B. subtilis
E. coli
PF-498 S. mutans MSEEEEVSEKVYNYLRRNEFFEVRKEE 723
E. coli FSA
PF-499 S. mutans VYSFLYVLVIVRKLLSMKKRIERL 724
E. coli
PF-500 S. mutans MGIFKEEKIKFIDCKGEEVILKIKIKDIKK 725
E. coli
PF-501 S. mutans GSTAHKSPIGSTNNQWGMKKTPTD 726
PF-502 S. mutans NKGKQMQDQTGKQPIVDNG 727
PF-503 S. mutans VVTLKDIVAVIEDQGYDVQ 728
PF-504 S. mutans ILSVELSTKTSASGS 729
E. coli
PF-505 S. mutans GYTKDPGTGI 730
PF-506 S. mutans SGRGFALIVVLFILLIIVGAACIR 731
E. coli
PF-507 S. mutans LALSIANLFKKKA 732
E. coli
PF-508 S. mutans VSTFGKVVKVVDEK 733
PF-509 S. mutans EAKVQAKGEQIACNNY 734
B. subtilis
E. coli
PF-510 S. mutans WYLYKKQSNQNDRGIPK 735
E. coli
PF-511 E. coli VMQSLYVKPPLILVTKLAQQN 736
P. aeruginosa
S. pneumoniae
C. jeikeium
PF-512 S. pneumoniae SFMPEIQKNTIPTQMK 737
C. jeikeium
PF-513 C. albicans SNGVGLGVGIGSGIRF-NH2 738
PF-514 S. epidermidis QRFYKLFYHIDLTNEQALKLFQVK 739
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-515 S. epidermidis DKSTQDKDIKQAKLLAQELGL-NH2 740
C. albicans
S. pneumoniae
C. jeikeium
PF-517 C. jejuni VKPTMTASLISTVC 741
PF-518 S. epidermidis SFYSKYSRYIDNLAGAIFLFF 742
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
PF-519 M. luteus YLVYSGVLATAAAF-NH2 743
E. faecalis
C. jeikeium
PF-520 S. epidermidis LGLTAGVAYAAQPTNQPTNQPTNQPTN 744
M. luteus QPTNQPTNQPRW-NH2
E. coli
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-521 S. epidermidis CGKLLEQKNFFLKTR 745
E. coli
P. aeruginosa
S. pneumoniae
E. faecalis
PF-522 S. epidermidis FELVDWLETNLGKILKSKSA-NH2 746
E. coli
P. aeruginosa
S. pneumoniae
E. faecalis
PF-523 S. epidermidis ASKQASKQASKQASKQASKQASRSLKN 747
M. luteus HLL
C. albicans
S. pneumoniae
C. jeikeium
C. jejuni
PF-524 S. epidermidis PDAPRTCYHKPILAALSRIVVTDR 748
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-526 S. epidermidis VLLLFIFQPFQKQLL-NH2 749
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-527 S. epidermidis GSVIKKRRKRMAKKKHRKLLKKTRIQR 750
M. luteus RRAGK
P. mirabilis
E. coli
P. aeruginosa
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-528 S. epidermidis LVDVVVLIRRHLPKSCS-NH2 751
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
PF-529 S. epidermidis LSEMERRRLRKRA-NH2 752
E. coli
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-537 S. epidermidis LANDYYKKTKKSW 753
M. luteus
P. mirabilis
E. coli
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-539 S. epidermidis SIILTKKKRRKIPLSIDSQIYKYTFKQ 754
M. luteus
B. subtilis
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-540 C. albicans KSILILIKVIFIGQTTIIL 755
PF-542 C. jeikeium KKDNPSLNDQDKNAVLNLLALAK 756
PF-543 S. epidermidis NILFGIIGFVVAMTAAVIVTAISIAK 757
M. luteus
B. subtilis
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-544 S. epidermidis FGEKQMRSWWKVHWFHP 758
M. luteus
P. mirabilis
P. aeruginosa
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-545 S. epidermidis RESKLIAMADMIRRRI-NH2 759
E. coli
P. aeruginosa
S. pneumoniae
E. faecalis
C. jeikeium
PF-546 S. epidermidis PIIAPTIKTQIQ 760
E. coli
C. albicans
S. pneumoniae
E. faecalis
C. jeikeium
PF-547 S. epidermidis WSRVPGHSDTGWKVWHRW-NH2 761
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
PF-548 M. luteus ARPIADLIHFNSTTVTASGDVYYGPG 762
P. mirabilis
E. coli
P. aeruginosa
C. albicans
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-549 E. coli TGIGPIARPIEHGLDS 763
C. albicans
S. pneumoniae
C. jeikeium
PF-550 S. pneumoniae STENGWQEFESYADVGVDPRRYVPL 764
PF-551 S. pneumoniae QVKEKRREIELQFRDAEKKLEASVQAE 765
PF-552 S. pneumoniae ELDKADAALGPAKNLAPLDVINRS 766
PF-553 S. epidermidis LTIVGNALQQKNQKLLLNQKKITSLG 767
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
C. jeikeium
PF-554 S. pneumoniae AKNFLTRTAEEIGEQAVREGNINGP 768
PF-555 MRSA EAYMRFLDREMEGLTAAYNVKLFTEAIS 769
S. pneumoniae
C. jeikeium
PF-556 S. epidermidis SLQIRMNTLTAAKASIEAA 770
M. luteus
B. fragilis
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
PF-557 S. pneumoniae AANKAREQAAAEAKRKAEEQAR 771
PF-558 S. epidermidis ADAPPPLIVRYS 772
E. coli
C. albicans
C. jeikeium
C. jejuni
PF-559 S. epidermidis SRPGKPGGVSIDVSRDRQDILSNYP 773
M. luteus
C. albicans
C. jeikeium
C. jejuni
PF-560 S. epidermidis FGNPFRGFTLAMEADFKKRK 774
M. luteus
E. coli
S. pneumoniae
C. jeikeium
C. jejuni
PF-562 S. epidermidis TPEQWLERSTVVVTGLLNRK 775
M. luteus
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-563 S. epidermidis RPELDNELDVVQNSASLDKLQASYN 776
M. luteus
C. jeikeium
PF-564 S. epidermidis TIILNDQINSLQERLNKLNAETDRR 777
C. albicans
S. pneumoniae
C. jeikeium
PF-566 P. mirabilis EAQQVTQQLGADFNAITTPTATKV 778
S. pneumoniae
PF-567 S. epidermidis QQRVKAVDASLSQVSTQVSGAVASA 779
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
C. jeikeium
PF-568 S. epidermidis TQAVQVKTAQAQQQ 780
PF-569 M. luteus KSKISEYTEKEFLEFVEDIYTNNK 781
P. mirabilis
S. pneumoniae
E. faecalis
C. jeikeium
PF-570 S. pneumoniae KKFPTEESHIQAVLEFKKLTEHPSG 782
C. jeikeium
PF-572 S. epidermidis WRASKGLPGFKAG 783
M. luteus
E. coli
S. pneumoniae
C. jeikeium
PF-573 S. epidermidis EKKLIVKLIDSIGKSHEEIVGAG 784
S. pneumoniae
PF-575 M. luteus LNFRAENKILEKIHISLIDTVEGSA 785
E. coli
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-576 M. luteus AYSGELPEPLVRKMSKEQVRSVMGK 786
P. mirabilis
E. coli
P. aeruginosa
C. albicans
S. pneumoniae
PF-577 S. epidermidis PFETRESFRVPVIGILGGWDYFMHP 787
M. luteus
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
PF-578 S. epidermidis QKANLRIGFTYTSDSNVCNLTFALLGSK 788
M. luteus
P. mirabilis
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-579 S. epidermidis MILVCAAVIWGRVLFILKFPIYFSIRLAFL 789
M. luteus
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-580 S. epidermidis EILNNNQVIKELTMKYKTQFESNLGGW 790
M. luteus TARARR
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-581 S. epidermidis WTARARR 791
M. luteus
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-583 S. epidermidis KFQGEFTNIGQSYIVSASHMSTSLNTGK 792
M. luteus
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-584 S. epidermidis SYIKNLSNQKFLIAF 793
M. luteus
P. mirabilis
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-585 S. epidermidis DYNHLLNVVQDWVNTN 794
E. coli
C. albicans
MRSA
S. pneumoniae
C. jeikeium
PF-586 S. epidermidis FFNQANYFFKEF 795
M. luteus
E. coli
P. aeruginosa
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-587 S. epidermidis ASGKYQSYLLNVYVDSKKDRLDIFDKL 796
M. luteus KAKAKFVL
E. coli
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-588 S. epidermidis ESVEAIKAKAIK 797
E. coli
C. albicans
E. faecalis
C. jeikeium
C. jejuni
PF-589 S. epidermidis APLRIDEIRNSNVIDEVLDCAPKKQEHFF 798
C. albicans VVPKIIE
MRSA
S. pneumoniae
PF-590 S. epidermidis YYQAKLFPLL 799
M. luteus
E. coli
E. faecalis
C. jeikeium
PF-592 S. epidermidis IMKNYKYFKLFIVKYALF 800
M. luteus
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-593 C. jeikeium MEISTLKKEKLHVKDELSQYLANYKK 801
PF-594 C. jeikeium IVSAIV 802
PF-595 S. epidermidis LQNKIYELLYIKERSKLCS 803
M. luteus
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-596 S. epidermidis SKMWDKILTILILILELIRELIKL 804
M. luteus
P. mirabilis
E. coli
P. aeruginosa
MRSA
E. faecalis
C. jeikeium
C. jejuni
PF-597 P. mirabilis DEIKVSDEEIEKFIKENNL 805
PF-598 S. epidermidis MKFMLEVRNKAISAYKEITRTQI 806
M. luteus
P. mirabilis
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
C. jeikeium
PF-599 S. epidermidis LFEIFKPKH 807
P. mirabilis
E. coli
C. albicans
MRSA
S. pneumoniae
C. jeikeium
PF-600 S. epidermidis TKKIELKRFVDAFVKKSYENYILERELK 808
M. luteus KLIKAINEELPTK
B. subtilis
P. mirabilis
E. coli
P. aeruginosa
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-601 C. jeikeium YRVTVKALE 809
PF-602 P. mirabilis LEKEKKEYIEKLFKTK 810
C. jeikeium
PF-603 S. epidermidis IDKLKKMNLQKLSYEVRISQDGKSIYAR 811
M. luteus IK
B. subtilis
E. coli
P. aeruginosa
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-604 S. epidermidis LMEQVEV 812
C. albicans
C. jeikeium
PF-605 S. epidermidis HYRWNTQWWKY 813
M. luteus
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-607 S. epidermidis YIESDPRKFDYIFGAIRDH 814
P. mirabilis
E. coli
MRSA
S. pneumoniae
C. jeikeium
PF-609 P. mirabilis TEIKLDNNEYLVLNLDDILGILK 815
E. coli
S. pneumoniae
PF-610 S. epidermidis VFLKLKTSKIDLASIIFYP 816
M. luteus
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
PF-612 S. epidermidis GTTLKYGLERQLKIDIHPEITIINLNGGA 817
M. luteus DEFAKL
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-613 C. jeikeium ADEFAKL 818
PF-614 S. epidermidis GLDIYA 819
E. coli
C. jeikeium
PF-615 S. epidermidis FLNRFIFYIFTVKTKSALIKNLFLD 820
M. luteus
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
C. jeikeium
C. jejuni
PF-616 C. jeikeium IVFVVTKEKK 821
PF-617 P. aeruginosa PMNAAEPE 822
C. albicans
PF-619 S. epidermidis WSRVPGHSDTGWKVWHRW 823
M. luteus
B. subtilis
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-621 S. epidermidis PPSSFLV 824
C. albicans
PF-622 S. epidermidis TREDVFSVRLINNIVNKQA 825
P. aeruginosa
C. albicans
S. pneumoniae
E. faecalis
C. jeikeium
PF-623 S. epidermidis VLFAVYLGALDWLFSWLTQKM 826
P. aeruginosa
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-625 S. epidermidis SDSTNNARTRKKARDVTTKDIDK 827
M. luteus
S. pneumoniae
C. jeikeium
PF-626 S. epidermidis KYDFDDFEPEEA 828
M. luteus
E. coli
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-627 S. epidermidis INDLLSYFTLHEK 829
P. aeruginosa
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-629 S. epidermidis GLAAIATVFALY 830
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-630 S. epidermidis IPATPIIHS 831
M. luteus
P. mirabilis
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-631 S. epidermidis LIIYFSKTGNTARATRQI 832
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-632 S. epidermidis TTIQGVASLEKHGFRYTIIYPTRI 833
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-634 S. epidermidis MPKARPVNHNKKKSKITIKSNFTLFYM 834
M. luteus FNP
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-635 S. epidermidis MNAHGHSLIFQKMIVHAFAFFSKQKNY 835
P. aeruginosa LYF
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-636 S. epidermidis LVRLA 836
C. albicans
MRSA
S. pneumoniae
E. faecalis
PF-637 S. epidermidis SRIKQDARSVRKYDRIGIFFYSFKSA 837
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-638 S. epidermidis TFILPK 838
C. albicans
MRSA
C. jeikeium
PF-639 S. pneumoniae QATQIKSWIDRLLVSED 839
C. jeikeium
PF-640 C. albicans MGDINRNF 840
PF-641 S. epidermidis SWKCHHLAIGGSWKCHHLAI 841
M. luteus
E. coli
C. albicans
MRSA
E. faecalis
C. jeikeium
C. jejuni
PF-642 M. luteus FTTPMIGIPAGLLGGSYYLKRREEKGK 842
MRSA
C. jeikeium
PF-643 Mycobacteria spp VRCRL 843
PF-644 Mycobacteria spp TSGLIIGENGLNGL 844
PF-645 Mycobacteria spp SNSVQQG 845
PF-646 Mycobacteria spp APASPGRRPG 846
PF-647 Mycobacteria spp GTFLGQKCAAATAS 847
PF-648 S. mutans ARRYPAAGS 848
E. coli
PF-649 Mycobacteria spp CPRYPFVDVGPAGPWRARWRVGS 849
PF-650 Mycobacteria spp IRSDQPGRQSRSSPRWPTGAGRHR 850
PF-651 Mycobacteria spp PRWPTGAGRHR 851
PF-652 Mycobacteria spp FLAPARPDLQAQRQALAQ 852
PF-653 Mycobacteria spp QSVHPLPAETPVADVI 853
PF-654 Mycobacteria spp LSGRLAGRR 854
PF-655 M. smegmatis DAPCFDDQFGDLKCQMC 855
PF-656 Mycobacteria spp RGMFVPFHDVDCVQ 856
PF-657 Mycobacteria spp YVANYTITQFGRDFDDRLAVAIHFA 857
PF-658 Mycobacteria spp PTTPPPTTPPEIPTGGTVIST 858
PF-659 Mycobacteria spp TVIST 859
PF-660 Mycobacteria spp TDPQATAAPRRRTSPR 860
PF-661 Mycobacteria spp PDEDIRRRAILPPAGPCRPMSPE 861
PF-662 Mycobacteria spp GKQSRAHGPVASRREFRRKSG 862
PF-663 Mycobacteria spp ATLIPRKA 863
PF-664 M. smegmatis DQLCVEYPARVSTG 864
PF-665 Mycobacteria spp VLRVATAVGEVPTGL 865
PF-666 Mycobacteria spp PNRRSRPR 866
PF-667 Mycobacteria spp PAHQRLRIDQRLVADRDMVQDYES 867
PF-668 Mycobacteria spp TNAESMALAFRGRVHMSVNIAGLT 868
PF-669 Mycobacteria spp RADRIESYPADGDRVITLWRNPYR 869
PF670 Mycobacteria spp TVIVAPMHSGV 870
PF-671 S. mutans TVSAFRTVH 871
E. coli
PF-673 S. mutans VRRLRM 872
E. coli
PF-674 S. mutans DGCDSEPALTYR 873
E. coli
PF-675 Mycobacteria spp EIIPISPTRRCEMHTMSSAEYRGL 874
PF-676 S. mutans AEYRGL 875
E. coli
PF-677 Mycobacteria spp TCRGAGMH 876
PF-678 Mycobacteria spp RDRRWTRRDMYDWLESARV 877
PF-679 S. mutans CRARFIRR 878
E. coli
PF-680 Mycobacteria spp ADPHPTTGI 879
PF-681 M. smegmatis TALTTVGVSGARLITYCVGVEDI 880
PF-682 Mycobacteria spp RRGKSEQGLSRR 881
PF-683 Mycobacteria spp LWPVA 882
PF-684 Mycobacteria spp RKLSLASGFALWRRSLV 883
PF-685 Mycobacteria spp PTLWLACL 884
PF-686 M. smegmatis LAVLMGYIGYRGWSGKRHINRQ 885
PF-687 Mycobacteria spp AKRVLSLAVAPHRRQPVQGT 886
PF-688 Mycobacteria spp ARNHAVIPAG 887
PF-689 S. mutans SAPSG 888
E. coli
PF-690 Mycobacteria spp MIPLAGDPVSSHRTVEFGVLGTYLVSG 889
GSL
PF-691 Mycobacteria spp HRTVEFGVLGTYLVSGGSL 890
PF-692 Mycobacteria spp GVAREDPLEPDPLAPIIDDSR 891
PF-693 Mycobacteria spp PDPAR 892
PF-694 Mycobacteria spp DLIRPLYSMSAPSVA 893
PF-695 Mycobacteria spp ALSVMLGNIPLVVPNANQL 894
PF-696 Mycobacteria spp IRSGISAAYARPLR 895
PF-697 Mycobacteria spp RADARAK 896
PF-698 Mycobacteria spp SSGRAGVKCRRPTGR 897
PF-699 Mycobacteria spp GRAGVKCRRPTGR 898
PF-700 Mycobacteria spp LNWPFTGR 899
PF-701 S. mutans PRGAQSGHG 900
PF-702 Mycobacteria spp LSGRLAGRR 901
PF-703 Mycobacteria spp MTTVDNIVGLVIAVALMAFLFAALLFPE 902
KF
PF-704 Mycobacteria spp APAARAAL 903
PF-705 S. mutans GEEEGTVAD 904
E. coli
PF-706 L. pneumophila LGYGAWIGCGLGLNGFHRID 905
PF-707 S. mutans IDPESIVTTNNKQDNVDEQ 906
E. coli
PF-709 S. mutans NKKHSPMD 907
PF-711 S. mutans KTAGPTGTIYKTN 908
PF-712 S. mutans QIYRHVHKVQAKSANLRLY 909
E. coli
PF-714 L. pneumophila FVVTQRMLRMYKK 910
PF-716 S. mutans HGENHHHKSDEKDNDSSEKKD 911
PF-717 E. coli PQSEVTFENIYAPKANGGGLYGI 912
PF-720 S. mutans SLDMGK 913
PF-724 L. pneumophila CYRFLTPKRPTRIS 914
PF-727 S. mutans AYARCRHDYPFTLGQMQTH 915
E. coli
PF-728 S. mutans AIGQEQDRREYYYYSGYPYYY 916
E. coli
PF-731 L. pneumophila RHKLIRLPLSESVFCFLNNPKI 917
PF-732 E. coli DRPSQTTHHTLSSSRITGPS 918
PF-733 S. mutans VISRQMGSEAVLELFIIM 919
E. coli
PF-735 S. mutans YDPLFPNDKN 920
E. coli
PF-737 S. epidermidis KSSGSSASASSTAGGSSSK 921
S. pneumoniae
PF-738 S. epidermidis KSGATSAASGAKSGASS 922
C. albicans
C. jeikeium
PF-741 S. epidermidis AKREDTVAAQIGANILNLIQ 923
M. luteus
P. mirabilis
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
PF-744 S. epidermidis LGVGTFVGKVLIKNQQKQKSKKKAQ 924
M. luteus
E. coli
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-745 S. epidermidis ANSQNSLFSNRSSFKSIFDKKSNITTNAT 925
M. luteus TPNSNIIIN
C. albicans
PF-746 S. epidermidis FLGNSQYFTRK 926
M. luteus
E. coli
C. albicans
S. pneumoniae
E. faecalis
C. jeikeium
PF-748 S. epidermidis FQGFFDVAVNKWWEEHNKAKLWKNV 927
M. luteus KGKFLEGEGEEEDDE
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-749 S. epidermidis GVNKWWEEHNKAKLWKNVKGKFLEG 928
M. luteus EGEEEDDE
E. coli
P. aeruginosa
C. albicans
S. pneumoniae
C. jeikeium
PF-750 M. luteus AESSPAKTTA 929
C. jeikeium
PF-751 S. epidermidis AESSPAQETT 930
E. coli
C. albicans
C. jeikeium
PF-752 S. epidermidis LHVIRPRPELSELKFPITKILKVNKQGLKK 931
E. coli
MRSA
S. pneumoniae
E. faecalis
PF-756 S. epidermidis DALLRLA 932
M. luteus
C. albicans
MRSA
C. jeikeium
PF-757 M. luteus PQAISSVQQNA 933
C. albicans
MRSA
PF-758 S. epidermidis PEIIKIVSGLL 934
M. luteus
E. coli
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-760 S. epidermidis DHITLDDYEIHDGFNFELYYG 935
M. luteus
PF-761 S. epidermidis SKFELVNYASGCSCGADCKCASETECK 936
M. luteus CASKK
P. mirabilis
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
PF-762 M. luteus PAPAPSAPAPAPEQPEQPA 937
C. albicans
PF-763 S. epidermidis GIWMARNYFHRSSIRKVYVESDKEYER 938
M. luteus VHPMQKIQYEGNYKSQ
E. coli
C. albicans
MRSA
S. pneumoniae
E. faecalis
PF-764 S. epidermidis GYFEPGKRD 939
M. luteus
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-765 S. epidermidis YLYWEVEHKPIIAKRDAYYAQLRKQKE 940
M. luteus IEEGA
E. coli
MRSA
E. faecalis
C. jeikeium
PF-766 S. epidermidis DAYYAQLRKQKEIEEGA 941
M. luteus
C. albicans
MRSA
E. faecalis
C. jeikeium
PF-767 S. epidermidis DGKQGEPVALKPTDN 942
M. luteus
E. coli
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-768 S. epidermidis GFRGGKRGGARG 943
S. pneumoniae
E. faecalis
C. jeikeium
PF-770 S. epidermidis GVGIGFIMMGVVGYAVKLVHIPIRYLIV 944
M. luteus
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
PF-772 S. epidermidis TKESSS 945
C. albicans
MRSA
S. pneumoniae
C. jeikeium
PF-773 S. epidermidis TLKESK 946
C. albicans
C. jeikeium
PF-776 S. epidermidis VSILLYLSATIILPNVLRLLVARAIIVRV 947
M. luteus
P. mirabilis
C. albicans
MRSA
S. pneumoniae
E. faecalis
PF-777 Mycobacteria spp. PGADGKLAEASAAIARLVRS 948
PF-778 Mycobacteria spp. MNLILTAHGT 949
PF-779 Mycobacteria spp. IYGDFFNFYLCDISLKVNGLQPGGPVRT 950
VKLFGQPTGRCTPQ
PF-780 Mycobacteria spp. AVYDALVALAAAEHRAELATRDARAK 951
DTYEKIGVHVVVAA
PF-781 Mycobacteria spp. PLVVVNHRRAERSRG 952
PF-782 Mycobacteria spp. TGPRRGIDLTSNRALSEVLDEGLELNSRK 953
PF-783 Mycobacteria spp. FTSEVRGVFTYRVNKAGLITNMRGYW 954
NLDMMTFGNQE
PF-784 Mycobacteria spp. MAMTTVDNIVGLVIAVALMAFLFAALL 955
FPEKF
PF-785 Mycobacteria spp. MRPQHSPAGKAFVVKKITHEQS 956
PF-786 Mycobacteria spp. LSERERRRLKRGII 957
PF-787 Mycobacteria spp. MTERQRRALLKQHPEVVSWSDYLEKR 958
KRRTGTAG
PF-788 Mycobacteria spp. GLITVFAGTARILQLRRAAKKTHAAALR 959
PF-789 Mycobacteria spp. PRGAQSGHG 960
PF-790 Mycobacteria spp. PAGPDHLDQRDHR 961
PF-791 S. mutans IFLTTQNTDYSEHNAA 962
PF-792 S. mutans ALHASGIQAI 963
PF-793 S. mutans YTQUNNASAYAMLLTNKDTVP 964
PF-794 S. mutans NLYFENQGN 965
PF-795 S. mutans ALHKSGIQVIADWVPDQIYN 966
PF-796 S. mutans YTQSNIPTAYALMLSNKDSI 967
PF-797 S. mutans WYYFDNNGYM 968
PF-798 S. mutans ALHSKGIKVMADWVPDQMYA 969
PF-799 S. mutans YTHYNTALSYALLLTNKSSVP 970
PF-800 S. mutans WYYFDNNGYM 971
PF-C003 A. naeslundii FCSVDHDVITIAADHVKQGAEA 972
P. gingivalis
S. mutans
PF-C008 A. naeslundii AQPRRTWLVNFGEVPSPGLTNDGMPDH 973
PF-C034 S. mutans HPMPITVRSRKPGPLTAPSEH 974
E. coli
PF-C045 A. naeslundii FREGMGWPLSNEGSPTAPLPKHRNQV 975
T. denticola
PF-C050 A. naeslundii QGLARPVLRRIPL 976
S. mutans
PF-C052 A. naeslundii SRFRNGV 977
F. nucleatum
S. mutans
PF-C055 A. naeslundii YNLSIYIYFLHTITIAGLITLPFII 978
F. nucleatum
P. gingivalis
S. mutans
PF-C057 A. naeslundii YFWWYWVQDCIPYKNNEVWLELSNN 979
F. nucleatum MK
P. gingivalis
S. mutans
PF-C058 A. naeslundii FETGFGDGYYMSLWGLNEKDEVCKVV 980
F. nucleatum IPFINPELID
P. gingivalis
S. mutans
PF-C061 A. naeslundii TLNYKKMFFSVIFLLGLNYLICNSPLFFK 981
F. nucleatum QIEF
P. gingivalis
S. mutans
T. denticola
PF-C062 A. naeslundii PLARATEVVATLFIICSLLLYLTR 982
F. nucleatum
P. gingivalis
S. mutans
T. denticola
PF-C063 A. naeslundii SHFRKGD 983
F. nucleatum
S. mutans
PF-C064 A. naeslundii DEEALEMGANLYAQFAIDFLNSKK 984
F. nucleatum
P. gingivalis
S. mutans
T. denticola
PF-C065 A. naeslundii DEERYSDSYFLKEKVFYLILALFLILFHQ 985
F. nucleatum KYLYFLEIITI
P. gingivalis
S. mutans
PF-C068 A. naeslundii LNLFASI 986
F. nucleatum
S. mutans
PF-C069 A. naeslundii NALMLREMQLAKNIKVEVTDVLSNKK 987
F. nucleatum YC
P. gingivalis
S. mutans
T. denticola
PF-C071 A. naeslundii QVIVKIL 988
F. nucleatum
S. mutans
PF-C072 A. naeslundii KKMFSLIRKVNWIFFILFIVLDLTNVFPLI 989
F. nucleatum RTILFAILSRQ
P. gingivalis
S. mutans
T. denticola
PF-C075 A. naeslundii KALVISVFAIVFSIIFVKFFYWRDKK 990
F. nucleatum
P. gingivalis
S. mutans
T. denticola
PF-C080 A. naeslundii INIPGLF 991
F. nucleatum
S. mutans
PF-C084 A. naeslundii FFSVIFLFGLNYLICNSPLFNILR 992
F. nucleatum
P. gingivalis
S. mutans
PF-C085 A. naeslundii KKFKIFVIINWFYHKYIILNFEENF 993
F. nucleatum
P. gingivalis
S. mutans
T. denticola
PF-C086 A. naeslundii ELFFTILSDCNELFLLHLLQQPLFYIKKGK 994
F. nucleatum
P. gingivalis
S. mutans
T. denticola
PF-C088 A. naeslundii DIANNILNSVSERLIIA 995
F. nucleatum
P. gingivalis
S. mutans
T. denticola
PF-C091 A. naeslundii ASNTPRFVRLTLFNFYSKIWNVTHLFLF 996
F. nucleatum NNL
P. gingivalis
S. mutans
T. denticola
PF-C093 A. naeslundii EKLGTMV 997
F. nucleatum
S. mutans
PF-C095 A. naeslundii LLALNMNEDTYYFELFFIFDNQNKKWL 998
F. nucleatum IFDLKERG
P. gingivalis
S. mutans
PF-C098 A. naeslundii PETKGKVSAFVFGIVVANVIAVVYILYM 999
F. nucleatum LREIGIIQ
P. gingivalis
S. mutans
T. denticola
PF-C120 A. naeslundii ASLSTMTFKVMELKELIILLCGLTMLMI 1000
F. nucleatum QTEFV
P. gingivalis
S. mutans
T. denticola
PF-C131 A. naeslundii QWIVAKREIRMHIYCHISVIHVIIFFG 1001
F. nucleatum
P. gingivalis
S. mutans
PF-C134 A. naeslundii NELMKYPATLTATATTPGIKYSHLCSVCL 1002
F. nucleatum
P. gingivalis
S. mutans
T. denticola
PF-C135 A. naeslundii KNTHAYLRVLRLSSLILSYQASVYPLFA 1003
F. nucleatum YLCQQKDY
P. gingivalis
S. mutans
PF-C136 A. naeslundii LILSYQASVYPLFAYLCQQKDY 1004
F. nucleatum
P. gingivalis
S. mutans
T. denticola
PF-C137 A. naeslundii QRMYWFKRGFETGDFSAGDTFAELK 1005
F. nucleatum
P. gingivalis
S. mutans
PF-C139 A. naeslundii LLASHPERLSLGVFFVYRVLHLLLENT 1006
F. nucleatum
P. gingivalis
S. mutans
T. denticola
PF-C142 A. naeslundii DFPPLSFFRRRFHAYTAPIDNFFGANPF 1007
F. nucleatum
P. gingivalis
S. mutans
T. denticola
PF-C143 A. naeslundii VVFGGGDRLV 1008
F. nucleatum
P. gingivalis
S. mutans
T. denticola
PF-C145 A. naeslundii YGKESDP 1009
F. nucleatum
P. gingivalis
S. mutans
T. denticola
PF-C160 F. nucleatum AASGFTYCASNGVWHPY 1010
PF-C180 F. nucleatum TVEELDKAFTWGAAAALAIGVIAINVG 1011
P. gingivalis LAAGYCYNNNDVF
S. mutans
T. denticola
PF-C181 P. gingivalis KMRAGQVVFIYKLILVLLFYVLQKLFD 1012
LKKGCF
PF-C194 A. naeslundii NTNDLLQAFELMGLGMAGVFIVLGILYI 1013
F. nucleatum VAELLIKIFPVNN
P. gingivalis
S. mutans
T. denticola
PF-C259 F. nucleatum AEIQPHCLSVL 1014
S. mutans
PF-C271 A. naeslundii FFPSYYSIIITYF 1015
F. nucleatum
P. gingivalis
S. mutans
T. denticola
PF-C273 A. naeslundii KNMLKRRMKQKRLFDEEDRLRVLSKY 1016
P. gingivalis TKSYY
S. mutans
T. denticola
PF-C281 A. naeslundii KKEKLLTAIRLQHRAEIRGYFTIFFLFFRI 1017
F. nucleatum
P. gingivalis
S. mutans
T. denticola
PF-C285 A. naeslundii FTIIELKKQKIKHGENNKKTAHPLNEPF 1018
F. nucleatum CARA
P. gingivalis
S. mutans
T. denticola
PF-C290 A. naeslundii GNVHPESDFHNLIQFIKTFLYFTIFFKYFL 1019
F. nucleatum
P. gingivalis
S. mutans
T. denticola
PF-C291 A. naeslundii HPFLTGTGCPLFLIFRLFFVKAYFSFTVF 1020
F. nucleatum
P. gingivalis
S. mutans
PF-S003 S. epidermidis ALALLKQDLLNFEGRGRIITSTYLQFNE 1021
M. luteus GCVP
P. mirabilis
E. coli
P. aeruginosa
C. albicans
MRSA
S. pneumoniae
E. faecalis
C. jeikeium
C. jejuni
M. smegmatis
PF-S004 S. epidermidis VLLNIFRTLLEFFSPSNAPGAEDVPLPDT 1022
MRSA QA
C. jeikeium
PF-S007 S. epidermidis VVAGVVLLTALAVGSKRKEKKQIKEIQ 1023
MRSA RLLAATR
PF-S015 S. epidermidis IENLERGARRPP 1024
MRSA
C. jeikeium
PF-S018 S. epidermidis GMPQIPRLRI 1025
M. luteus
C. albicans
MRSA
E. faecalis
C. jeikeium
C. jejuni
PF-S023 S. epidermidis MAEDERRALKRRTNRGRTRTRKRITV 1026
MRSA
PF-S026 S. epidermidis TELKYNGEEYLLLTQRDILAVIEK 1027
MRSA
C. jeikeium
PF-S029 M. luteus TSDTQSQSPWLFDNADIVNIYPVQLMHS 1028
P. mirabilis SDND
E. coli
C. albicans
C. jeikeium
C. jejuni
* Peptide binding was conducted in aqueous buffers that varied depending on peptide solubility. For example: Brain Heart Infusion (BHI) Media; 1X Phosphate-buffered saline (PBS); 0.05% v/v Tween-20; 0.05% v/v Tween-80; 1% v/v Glycerol; 50 μM Guanidine hydrochloride; 0.05% v/v Acetic acid; 50 μM Urea; 1% v/v Polyethylene glycol 400 (PEG 400); 20 mM Sodium glutamate; 50 mM Piperazine-1,4-bis(2-ethanesulfonic acid) (PIPES); 50 mM Sodium acetate; 1% v/v Pluronic 17R4; 1% w/v Pluronic F108; 1% w/v Pluronic P123; 0.2% v/v Cetyl trimethylammonium bromide (CTAB); 0.8% v/v β-D-Octyl glucoside (BOG); 0.2% CTAB and 0.05% Tween-20; 0.2% CTAB and 0.05% Tween-80; 0.2% CTAB and 1% glycerol; and 20 mM HEPES (4-(2-hydroxyethyl)-1- piperazineethanesulfonic acid), 150 mM sodium chloride, 1 mM magnesium chloride and 0.1% CTAB. Preferably, binding was evaluated in 1x PBS.
** Three-amino acid code: Dab: Diaminobutyric acid; Orn: Ornithine; cDOrn, cOrn: side-chain cyclical Ornithine; Abreviations: c(X . . . Y) indicates amino acids are cyclic, connected X to Y; DX indicates D-isoform amino acids.
In certain embodiments, the amino acid sequence of the targeting peptides comprises or consists of a single amino acid sequence, e.g., as listed above in Table 3. In certain embodiments the amino acid sequence of the targeting peptides comprises two copies, three copies, four copies, five copies six copies or more of one or more of the amino acid sequences listed in Table 3, and/or Table 10, and/or Table 12. Thus, compound targeting constructs are contemplated where the construct comprises multiple domains each having targeting activity. The targeting domains comprising such a construct can be the same or different. In certain embodiments the construct comprises at least 2, at least 3, at least 4, at least 5, at least 6, at least 7, or at least 8 different targeting domains each domain comprising a different targeting sequence.
Various targeting domains comprising such a construct can be joined directly to each other or two or more of such domains can be attached to each other via a linker. An illustrative, but non-limiting, list of suitable linkers is provided in Table 16. Thus, in certain embodiments, two or more targeting domains comprising a compound/multiple targeting construct are chemically conjugated together.
In certain embodiments the two or more targeting domains comprising the construct are joined by a peptide linker. Where all the targeting domains are attached directly to each other or are joined by peptide linkers, the entire construct can be provided as a single-chain peptide (fusion protein).
In various embodiments, the targeting peptides described herein comprise one or more of the amino acid sequences shown in Table 3, and/or Table 10, and/or Table 12 (and/or the retro, inverso, retroinverso, etc. forms of such sequences). In certain embodiments the peptides range in length up to about 100 amino acids in length, preferably up to about 80, about 70, about 60, or about 51 amino acids in length. In certain embodiments the peptides range in length from about 8 amino acids up to about 100 amino acids 80 amino acids, 60 amino acids or about 51 amino acids in length. In certain embodiments the peptides range in length from about 8 up to about 50, 40, 30, 20, 15, 15, 13, or 12 amino acids in length.
As shown in Tables 3, 10, and 12 the various amino acid sequences described herein target particular microorganisms. The range of activity of the peptides or compositions comprising such peptides can be increased by including amino acid sequences that target different microorganisms either as separate components and/or as multiple domains within a single construct.
In some embodiments greater specificity and/or avidity can be obtained by including multiple different amino acid sequences that target the same microorganism.
II. Antimicrobial Peptides. A) Uses of Antimicrobial Peptides.
The antimicrobial peptides described herein also have a wide variety of uses. For example, the peptides can be formulated individually, in combination, in combination with other antimicrobial peptides, and/or in combination with various antibacterial agents to provide antimicrobial pharmaceuticals.
In various embodiments, the antimicrobial peptides described herein can be formulated individually, in combination, in combination with other antimicrobial peptides, and/or in combination with various antibiotic (e.g., antibacterial) agents in “home healthcare” formulations. Such formulations include, but are not limited to toothpaste, mouthwash, tooth whitening strips or solutions, contact lens storage, wetting, or cleaning solutions, dental floss, toothpicks, toothbrush bristles, oral sprays, oral lozenges, nasal sprays, aerosolizers for oral and/or nasal application, wound dressings (e.g., bandages), and the like.
In various embodiments the antimicrobial peptides described herein can be formulated individually, in combination, in combination with other antimicrobial peptides, and/or in combination with various antibiotic (e.g., antibacterial) agents in various cleaning and/or sterilization formulations for use in agriculture, in fool preparation and transport, in the home, workplace, clinic, or hospital.
In certain embodiments the antimicrobial peptides described herein are attached to one or more targeting moieties to specifically and/or to preferentially deliver the peptide(s) to a target (e.g. a target microorganism, biofilm, bacterial film, particular tissue, etc.).
Other possible uses of the targeting and/or antimicrobial peptides disclosed herein include, but are not limited to biofilm dispersal, biofilm retention, biofilm formation, anti-biofilm formation, cell agglutination, induction of motility or change in motility type, chemoattractant or chemorepellent, extracellular signal for sporogenesis or other morphological change, induction or inhibition of virulence gene expression, utilized as extracellular scaffold, adhesin or binding site, induction or suppression of host immune response, induction or suppression of bacterial/fungal antimicrobial molecule production, quorum-sensing, induction of swarming behavior, apoptosis or necrosis inducing in eukaryotic cells, affecting control of or inducing the initiation of cell cycle in eukaryotes, in archaea or prokaryotes, induces autolysis or programmed cell death, inhibition of phage/virus attachment or replication, evasion of innate immunity, induction or inhibition of genetic transformation or transduction competence, induction or inhibition of pilus-mediated conjugation, induction or inhibition of mating behavior in bacteria and fungi, induction or inhibition of nodule formation or metabolic compartmentalization, metal, ion, or nutrient binding, acquisition or inhibition of metal, ion, or nutrient binding and acquisition, and the like.
In certain embodiments, compositions and methods are provided for decreasing the infectivity, morbidity, and rate of mortality associated with a variety of pathogens. The present invention also relates to methods and compositions for decontaminating areas, samples, solutions, and foodstuffs colonized or otherwise infected by pathogens and microorganisms. Certain embodiments of the present compositions are nontoxic and may be safely ingested by humans and other animals. Additionally, certain embodiments of the present invention are chemically stable and non-staining.
In some embodiments, the present invention provides compositions and methods suitable for treating animals, including humans, exposed to pathogens or the threat of pathogens. In some embodiments, the animal is contacted with effective amounts of the compositions prior to exposure to pathogenic organisms. In other embodiments, the animal or human is contacted with effective amounts of the compositions after exposure to pathogenic organisms. Thus, the present invention contemplates both the prevention and treatment of microbiological and other infections.
In certain embodiments compositions and methods are provided for decontaminating solutions and surfaces, including organic and inorganic samples that are exposed to pathogens or suspected of containing pathogens. In still other embodiments of the present invention, the compositions are used as additives to prevent the growth of harmful or undesired microorganisms in biological and environmental samples.
These applications of the peptides described herein are intended to be illustrative and not limiting. Using the teaching provided herein, other uses will be recognized by one of skill in the art.
B Illustrative Novel Antimicrobial Peptides.
Antimicrobial peptides (also called host defense peptides) are an evolutionarily conserved component of the innate immune response and are found among all classes of life. Unmodified, these peptides are potent, broad spectrum antibiotics which demonstrate potential as novel therapeutic agents. Antimicrobial peptides have been demonstrated to kill Gram-negative and Gram-positive bacteria (including strains that are resistant to conventional antibiotics), mycobacteria (including Mycobacterium tuberculosis), enveloped viruses, and fungi.
Naturally-occurring antimicrobial peptides are typically short peptides, generally between 12 and 50 amino acids. These peptides often include two or more positively charged residues provided by arginine, lysine or, in acidic environments, histidine, and frequently a large proportion (generally >50%) of hydrophobic residues (see, e.g., Papagianni et al. (2003) Biotechnol Adv 21: 465; Sitaram and Nagaraj (2002) Curr Pharm Des 8: 727; Dürr et al. (2006) Biochim. Biophys. Acta 1758: 1408-1425).
Frequently the secondary structures of these molecules follow 4 themes, including i) α-helical, ii) β-stranded due to the presence of 2 or more disulfide bonds, iii) β-hairpin or loop due to the presence of a single disulfide bond and/or cyclization of the peptide chain, and iv) extended. Many of these peptides are unstructured in free solution, and fold into their final configuration upon partitioning into biological membranes. The ability to associate with membranes is a definitive feature of antimicrobial peptides although membrane permeabilisation is not necessary. These peptides have a variety of antimicrobial activities ranging from membrane permeabilization to action on a range of cytoplasmic targets.
The modes of action by which antimicrobial peptides kill bacteria is varied and includes, but is not limited to disrupting membranes, interfering with metabolism, and targeting cytoplasmic components. In many cases the exact mechanism of killing is not known.
In certain embodiments the antimicrobial peptides include peptides comprising or consisting of one or more of the amino acid sequences shown in Tables 4 (SEQ ID NOs:1029-1078), and/or Table 5 (SEQ ID NOs:1079-1566). In various embodiments the peptides include peptides comprising or consisting of the retro, inverso, retro-inverso, and/or beta form of one or more of the amino acid sequences shown in Tables 4 (SEQ ID NOs:1029-1078), and/or Table 5 (SEQ ID NOs:1079-1566). The peptides can comprise all “L” amino acids, all “D” amino acids, or combinations of “L” and “D” amino acids. Also contemplated are circular permutations of these sequences as well as peptides comprising or consisting of the retro, inverso, retro-inverso, and/or beta form of such circular permutations.
It will also be recognized, that in certain embodiments, any peptide or compound AMP described herein can be circularized.
In various embodiments the peptides can optionally bear one or more protecting groups, e.g., and the amino and/or carboxyl termini, and/or on side chains.
Also contemplated are peptides comprising one, two, three four, or five conservative substitutions of these amino acid sequences.
TABLE 4
Novel antimicrobial peptides, target
microorganisms and MIC values.
Organism MIC SEQ
ID (μM) Structure/sequence ID NO
K-1 S. mutans, 25 GLGRVIGRLIKQIIWRR 1029
K-2 S. mutans, 12.5 VYRKRKSILKIYAKLKGWH 1030
K-7 S. mutans, 12.5 NYRLVNAIFSKIFKKKFIKF 1031
K-8 S. mutans, 4 KILKFLFKKVF 1032
K-9 S. mutans, 4 FIRKFLKKWLL 1033
K-10 S. mutans, 4 KLFKFLRKHLL 1034
K-11 S. mutans, 4 KILKFLFKQVF 1035
K-12 S. mutans, 8 KILKKLFKFVF 1036
K-13 S. mutans, 16 GILKKLFTKVF 1037
K-14 S. mutans, 8 LRKFLHKLF 1038
K-15 S. mutans, 4 LRKNLRWLF 1039
K-16 S. mutans, 8 FIRKFLQKLHL 1040
P. aeruginosa, 12.5
MRSA , 25
K-17 S. mutans, 8 FTRKFLKFLHL 1041
K-18 S. mutans, 16 KKFKKFKVLKIL 1042
K-19 S. mutans, 16 LLKLLKLKKLKF 1043
K-20 S. mutans, 8 FLKFLKKFFKKLKY 1044
K-21 S. mutans, 8 GWLKMFKKIIGKFGKF 1045
K-22 S. mutans, 8 GIFKKFVKILYKVQKL 1046
1T-88 GRLVLEITADEVKALGEALANAKI 1047
PF-531 A. baumannii, 25 YIQFHLNQQPRPKVKKIKIFL-NH2 1048
P. aeruginosa, 50
T. rubrum, 50
A. niger, 25
B. subtilis, 25
C. difficile, 12.5
C. jeikeium, 6.25
S. epidermidis, 50
S. mutans, 12.5
PF-527 P. aeruginosa, 50 GSVIKKRRKRMAKKKHRKLLKKTRIQR 1049
T. rubrum, 25 RRAGK
A. niger, 50
B. subtilis, 12.5
C. jeikeium, 6.25
MRSA , 50
S. epidermidis, 25
PF-672 C. albicans, 1.56 MRFGSLALVAYDSAIKHSWPRPSSVRR 1050
T. rubrum, 0.78 LRM
A. niger, 3
B. subtilis, 0.78
E. faecalis, 3.13
MRSA , 1.56
S. epidermidis, 0.39
PF-606 E. coli, 50 FESKILNASKELDKEKKVNTALSFNSHQ 1051
MRSA , 50 DFAKAYQNGKI
S. epidermidis, 50
S. mutans, 50
S. pneumoniae, 50
PF-547 T. rubrum, 25 WSRVPGHSDTGWKVWHRW-NH2 1052
B. subtilis, 25
S. mutans, 12.5
PF-006 A. baumannii, 50 MGIIAGIIKFIKGLIEKFTGK 1053
B. subtilis, 25
MRSA , 50
PF-545 A. niger, 50 RESKLIAMADMIRRRI-NH2 1054
B. subtilis, 25
MRSA , 50
PF-278 C. albicans, 50 LSLATFAKIFMTRSNWSLKRFNRL 1055
T. rubrum, 50
S. epidermidis, 50
PF-283 T. rubrum, 50 MIRIRSPTKKKLNRNSISDWKSNTSGRF 1056
B. subtilis, 50 FY
S. epidermidis, 50
PF-307 C. albicans, 50 MKRRRCNWCGKLFYLEEKSKEAYCCK 1057
T. rubrum, 50 ECRKKAKKVKK
B. subtilis, 50
PF-168 T. rubrum, 50 VLPFPAIPLSRRRACVAAPRPRSRQRAS 1058
A. niger, 50
MRSA , 50
PF-538 A. baumannii, 25 KNKKQTDILEKVKEILDKKKKTKSVGQ 1059
C. difficile, 25 KLY
PF-448 A. niger, 25 SLQSQLGPCLHDQRH 1060
S. pneumoniae, 50
PF-583 MRSA , 50 KFQGEFTNIGQSYIVSASHMSTSLNTGK 1061
S. epidermidis, 50
PF-600 E. coli, 50 TKKIELKRFVDAFVKKSYENYILERELK 1062
S. pneumoniae, 50 KLIKAINEELPTK
PF-525 A. niger, 50 KFSDQIDKGQDALKDKLGDL 1063
S. pneumoniae, 50
PF-529 A. niger, 50 LSEMERRRLRKRA-NH2 1064
S. pneumoniae, 50
PF-148 A. niger, 50 RRGCTERLRRMARRNAWDLYAEHFY 1065
B. subtilis, 50
PF-530 A. baumannii, 25 SKFKVLRKIIIKEYKGELMLSIQKQR 1066
PF-522 C. difficile, 25 FELVDWLETNLGKILKSKSA-NH2 1067
PF-497 B. subtilis, 50 LVLRICTDLFTFIKWTIKQRKS 1068
PF-499 B. subtilis, 50 VYSFLYVLVIVRKLLSMKKRIERL 1069
PF-322 B. subtilis, 50 GIVLIGLKLIPLLANVLR 1070
PF-511 S. pneumoniae, 50 VMQSLYVKPPLILVTKLAQQN 1071
PF-512 S. pneumoniae, 50 SFMPEIQKNTIPTQMK 1072
PF-520 S. pneumoniae, 50 LGLTAGVAYAAQPTNQPTNQPTNQPTN 1073
QPTNQPTNQPRW-NH2
PF-521 S. pneumoniae, 50 CGKLLEQKNFFLKTR 1074
PF-523 S. pneumoniae, 50 ASKQASKQASKQASKQASKQASRSLKN 1075
HLL
PF-524 S. pneumoniae, 50 PDAPRTCYHKPILAALSRIVVTDR 1076
PF-209 MRSA , 50 NYAVVSHT 1077
PF-437 S. pneumoniae, 50 FQKPFTGEEVEDFQDDDEIPTII 1078
Where protecting groups are shown (e.g., —NH2) they are optional. Conversely any peptide shown without protecting groups can bear one or more such groups.
In certain embodiments peptides that induce alterations in phenotype or other biological activities can also be used as antimicrobial effector moieties. Illustrative alternative peptides are shown in Table 5.
TABLE 5
Illustrative list of novel morphology, biofilm
and growth disrupting peptides.
SEQ ID
ID Organism, effect Structure/sequence NO
G-1 S. mutans: Ca2+ DSSQSDSDSDSNSSNTNSNSSITNG 1079
binding
G-2 S. mutans: biofilm LPGTLHIQAEFPVQLEAGSLIQIFD 1080
structure
G-4 S. mutans: EIPIQLANDLANYYDISLDSIFFW 1081
Biofilm structure
G-5 M. xanthus: RDMTVAGKRPNFLIITTDEE 1082
Altered cell
morphology
G-6 M. xanthus: NTSIVCAVTFAPIKEVPLLWRAGLTLRS 1083
Altered cell RQS
morphology
G-7 M. xanthus: QAKVEREVERDLVYTLRRLCDPSGSER 1084
Altered cell TK
morphology
G-8 S. mutans: PRMIDIISFHGCHGDHQVWTDPQATAL 1085
Altered biofilm PR
structure
PF-001 S. epidermidis (C) MNNWIIVAQLSVTVINEIIDIMKEKQKG 1086
M. luteus (C) GK
MRSA (R)
C. jeikeium (D)
PF-002 B. subtilis (R) NDDAQ 1087
S. pneumoniae (H)
PF-003 S. epidermidis (D) MNNWIKVAQISVTVINEVIDIMKEKQN 1088
M. luteus (A) GGK
MRSA (R)
C. jeikeium (A)
PF-004 S. epidermidis (A) ARLSKAIIIAVIVVYHLDVRGLF 1089
M. luteus (A)
MRSA (R)
C. jeikeium (A)
PF-005 B. subtilis (C) MESIFKIKLMNGICRSENMNMKKKNK 1090
S. pneumoniae (H) GEKI
PF-006 S. epidermidis (D) MGIIAGIIKFIKGLIEKFTGK 1091
M. luteus (A)
B. subtilis (I)
MRSA (I)
S. pneumoniae (R)
C. jejuni (D)
PF-007 S. epidermidis (A) MGIIAGIIKVIKSLIEQFTGK 1092
M. luteus (A)
E. coli (A)
MRSA (R)
E. faecalis (A)
PF-008 B. subtilis (D) MIEIGSIAYLNGGSKKYNHILNQENR 1093
C. jejuni (R)
PF-009 S. epidermidis (S) SKKYNHILNQENR 1094
PF-010 S. epidermidis (S) MDIDVNKLLQAFVYFKSFEKLRHNNS 1095
M. luteus (A)
MRSA (R)
C. jeikeium (A)
PF-011 MRSA (R) MFCYYKQHKGDNFSIEEVKNIIADNEM 1096
C. jeikeium (C) KVN
PF-012 S. epidermidis (S) WRGPNTEAGGKSANNIVQVGGAPT 1097
M. luteus (C)
MRSA (R)
C. jeikeium (A)
PF-013 S. epidermidis (C) LIQKGLNQTFIVVIRLNNFIKKS 1098
M. luteus (D)
MRSA (R)
C. jeikeium (D)
PF-015 MRSA (W) SIDKRNLYNLKYYE 1099
PF-017 MRSA (M) ESIIE 1100
PF-019 MRSA (M) NDTNK 1101
PF-020 S. mutans (F) MKIILLLFLIFGFIVVVTLKSEHQLTLFSI 1102
S. epidermidis (C)
M. luteus (C)
MRSA (C)
S. pneumoniae (D)
PF-021 S. epidermidis (A) FSLNFSKQKYVTVN 1103
M. luteus (A)
MRSA (R)
C. jeikeium (R)
PF-022 S. epidermidis (D) MINELKNKNSGIMNNYVVTKESKL 1104
M. luteus (A)
MRSA (R)
C. jeikeium (A)
PF-023 MRSA (S) MTKNTIISLENEKTQINDSENESSDLRK 1105
AK
PF-024 S. epidermidis (D) DLRKAK 1106
MRSA (M)
PF-025 S. epidermidis (S) LLIIFRLWLELKWKNKK 1107
M. luteus (A)
MRSA (R)
C. jeikeium (A)
PF-026 MRSA (M) SIHFIN 1108
PF-027 S. epidermidis (D) HNARKYLEFISQKIDGDKLTKEDSL 1109
MRSA (M)
PF-028 S. epidermidis (M) ALDCSEQSVILWYETILDKIVGVIK 1110
MRSA (R)
C. jeikeium (M)
PF-029 MRSA (M) NSTNE 1111
PF-030 S. epidermidis (D) MTCHQAPTTTHQSNMA 1112
M. luteus (C)
MRSA (R)
C. jeikeium (C)
PF-031 MRSA (M) MPHHSTTSSRIVVPAHQSNMASTPNLSI 1113
TP
PF-032 S. epidermidis (S) RIVVPAHQSNMASTPNLSITP 1114
C. jeikeium (C)
PF-033 S. epidermidis (M) MFIFKTTSKSHFHNNVKSLECIKIPINK 1115
B. subtilis (C) NR
MRSA (M)
S. pneumoniae (R)
C. jeikeium (D)
C. jejuni (R)
PF-034 S. epidermidis (A) EPKKKHFPKMESASSEP 1116
PF-035 MRSA (M) SFYESY 1117
PF-036 S. epidermidis (S) ILNRLSRIVSNEVTSLIYSLK 1118
M. luteus (A)
MRSA (R)
C. jeikeium (A)
PF-037 S. epidermidis (D) MTKKRRYDTTEFGLAHSMTAKITLHQ 1119
M. luteus (C) ALYK
MRSA (R)
C. jeikeium (D)
PF-040 S. mutans (F) MIHLTKQNTMEALHFIKQFYDMFFILN 1120
S. epidermidis (D) FNV
M. luteus (D)
B. subtilis (D)
P. mirabilis (C)
E. coli (C)
MRSA (D)
S. pneumoniae (D)
C. jeikeium (D)
C. jejuni (D)
PF-041 S. epidermidis (R) ELLVILPGFI 1121
MRSA (M)
PF-042 S. epidermidis (D) LLLSYFRYTGALLQSLF 1122
M. luteus (C)
MRSA (R)
C. jeikeium (S)
PF-043 S. epidermidis (D) MIKNETAYQMNELLVIRSAYAK 1123
M. luteus (C)
MRSA (R)
C. jeikeium (A)
PF-045 MRSA (S) LDINDYRSTY 1124
PF-046 S. epidermidis (C) LDFYLTKHLTLML 1125
MRSA (R)
C. jeikeium (R)
PF-048 S. epidermidis (D) LYFAFKKYQERVNQAPNIEY 1126
MRSA (W)
C. jeikeium (S)
PF-049 MRSA (S) AYYLKRREEKGK 1127
PF-051 S. mutans (D) RFFNFEIKKSTKVDYVFAHVDLSDV 1128
S. epidermidis (D)
M. luteus (C)
MRSA (D)
S. pneumoniae (D)
PF-052 S. epidermidis (S) QELINEAVNLLVKSK 1129
M. luteus (A)
MRSA (R)
C. jeikeium (D)
PF-053 S. epidermidis (C) KLFGQWGPELGSIYILPALIGSIILIAIVT 1130
M. luteus (D) LILRAMRK
B. subtilis (H)
E. coli (A)
P. aeruginosa (A)
C. albicans (A)
MRSA (D)
S. pneumoniae (S)
E. faecalis (A)
C. jeikeium (D)
C. jejuni (D)
PF-056 S. epidermidis (D) AEQLFGKQKQRGVDLFLNRLTIILSILF 1131
M. luteus (D) FVLMICISYLGM
B. subtilis (C)
C. albicans (B)
MRSA (M)
S. pneumoniae (D)
C. jeikeium (S)
C. jejuni (D)
PF-057 S. epidermidis (D) TMIVISIPRFEEYMKARHKKWM 1132
M. luteus (C)
E. coli (M)
C. albicans (A)
MRSA (M)
S. pneumoniae (R)
E. faecalis (A)
C. jeikeium (A)
C. jejuni (D)
PF-058 MRSA (M) FADQSQDNA 1133
PF-059 C. jejuni (C) TITLKAGIERALHEEVPGVIEVEQVF 1134
PF-061 S. epidermidis (R) GYNSYKAVQDVKTHSEEQRVTAKK 1135
B. subtilis (R)
S. pneumoniae (R)
C. jejuni (R)
PF-063 S. epidermidis (R) IAAIIVLVLFQKGLLQIFNWILIQLQ 1136
M. luteus (R)
B. subtilis (C)
P. aeruginosa (A)
MRSA (M)
S. pneumoniae (D)
C. jeikeium (D)
C. jejuni (D)
PF-064 S. epidermidis (D) DYYGKE 1137
MRSA (M)
PF-065 S. epidermidis (D) LEKNTRDNYFIHAIDRIYINTSKGLFPES 1138
MRSA (R) ELVAWG
C. jeikeium (A)
PF-066 MRSA (S) IKGTVKAVDETTVVITVNGHGTELTFE 1139
KPAIKQVDPS
PF-067 S. epidermidis (D) DLIVKVHICFVVKTASGYCYLNKREAQ 1140
M. luteus (R) AAI
B. subtilis (C)
P. aeruginosa (A)
MRSA (M)
S. pneumoniae (D)
C. jeikeium (D)
C. jejuni (D)
PF-068 S. epidermidis (M) SHLINNFGLSVINPSTPICLNFSPVFNLL 1141
M. luteus (D) TVYGITCN
B. subtilis (A)
E. coli (A)
MRSA (M)
S. pneumoniae (D)
E. faecalis (A)
C. jeikeium (R)
C. jejuni (D)
PF-069 B. subtilis (D) FDPVPLKKDKSASKHSHKHNH 1142
C. jejuni (R)
PF-070 B. subtilis (D) SMVKSEIVDLLNGEDNDD 1143
PF-071 S. epidermidis (R) HCVIGNVVDIANLLKRRAVYRDIADVI 1144
M. luteus (R) KMR
B. subtilis (D)
C. albicans (B)
MRSA (C)
S. pneumoniae (A)
C. jejuni (A)
PF-073 S. epidermidis (R) CPSVTMDACALLQKFDFCNNISHFRHF 1145
M. luteus (R) FAIKQPIER
MRSA (M)
S. pneumoniae (D)
C. jeikeium (D)
C. jejuni (D)
PF-074 S. epidermidis (D) RDIHPIYFMTKD 1146
MRSA (M)
PF-075 S. epidermidis (D) FVNSLIMKDLSDNDMRFKYEYYNREK 1147
M. luteus (A) DT
MRSA (R)
C. jeikeium (D)
PF-076 S. epidermidis (S) LYQYELLSKEEYLKCTLIINQRRNEQK 1148
M. luteus (A)
MRSA (R)
C. jeikeium (A)
PF-099 S. epidermidis (D) EIIAYLEGRFANA 1149
C. jeikeium (C)
PF-123 S. epidermidis (M) TTRPQVAEDRQLDDALKETFPASDPISP 1150
PF-124 S. epidermidis (C) MADGQIAAIAKLHGVPVATRNIRHFQS 1151
C. jeikeium (R) FGVELINPWSG
PF-125 S. epidermidis (D) YVVGALVILAVAGLIYSMLRKA 1152
M. luteus (C)
PF-127 S. epidermidis (M) MLRYLSLFAVGLATGYAWGWIDGLA 1153
M. luteus (A) ASLAV
C. jeikeium (A)
PF-128 S. epidermidis (D) GIKVVAARFEEIQFSENFDSIILA 1154
P. aeruginosa (C)
PF-129 S. epidermidis (M) MKLLARDPWVCAWNDIW 1155
C. jeikeium (R)
PF-133 C. jeikeium (R) GDPTAGQKPVECP 1156
PF-135 C. jeikeium (R) PPARPARIPQTPTLHGASLFRQRS 1157
PF-137 S. epidermidis (D) VLGKGHDLLDVGKTALKSRVFAWLG 1158
M. luteus (D) GS
C. jeikeium (A)
PF-139 S. epidermidis (M) ALSKPAIQARTLCRRQDPP 1159
M. luteus (C)
C. jeikeium (R)
PF-140 S. epidermidis (D) FHRRVIRASEWALTTRSFSTPLRSAAR 1160
M. luteus (R)
P. aeruginosa (A)
C. albicans (B)
MRSA (M)
S. pneumoniae (D)
C. jeikeium (D)
C. jejuni (D)
PF-143 P. aeruginosa (C) LSPRPIIVSRRSRADNNNDWSR 1161
PF-144 S. pneumoniae (H) RSGQPVGRPSRRAWLR 1162
PF-145 S. epidermidis (D) GIVLTGRAGLVSGACSMALGVGLG 1163
M. luteus (A)
B. subtilis (C)
MRSA (M)
S. pneumoniae (R)
C. jeikeium (R)
C. jejuni (R)
PF-148 S. epidermidis (D) RRGCTERLRRMARRNAWDLYAEHFY 1164
M. luteus (A)
B. subtilis (I)
C. albicans (B)
MRSA (C)
S. pneumoniae (R)
C. jeikeium (H)
C. jejuni (H)
PF-149 MRSA (H) GKVSVLTRVPRSLGGAPANQ 1165
PF-153 S. epidermidis (M) GILARADCSQIA 1166
C. jeikeium (C)
PF-156 MRSA (H) LITAEQPATAPIAGK 1167
PF-157 S. epidermidis (M) HTAVVWLAGVSGCVALSHCEPA 1168
PF-164 C. jeikeium (R) EEVSRALAGIGLGLGCRIG 1169
PF-168 P. aeruginosa (H) VLPFPAIPLSRRRACVAAPRPRSRQRAS 1170
MRSA (I)
PF-171 S. epidermidis (R) TQVTLCRTW 1171
M. luteus (R)
B. subtilis (D)
MRSA (M)
S. pneumoniae (D)
C. jejuni (R)
PF-173 S. epidermidis (A) AGRTAIVQGGG 1172
C. jeikeium (D)
PF-175 M. luteus (S) RRRPAGQRPEKASQAMIAA 1173
B. subtilis (D)
C. albicans (B)
S. pneumoniae (A)
C. jejuni (M)
PF-176 S. epidermidis (C) RLTSNQFLTRITPFVFAQH 1174
M. luteus (C)
C. jeikeium (D)
PF-178 S. epidermidis (D) EVYSSPTNNVAITVQNN 1175
E. coli (C)
MRSA (M)
S. pneumoniae (D)
PF-180 S. epidermidis (C) SGLGDLGFSSEAK 1176
PF-186 S. epidermidis (C) DADKNLSLERDRFAWRVAAP 1177
C. jeikeium (A)
PF-188 C. jeikeium (H) ARTFAGRLGTRYFGGLMRSTKA 1178
PF-190 S. epidermidis (C) HFILRKPLLFMIHSLKTGPLDRF 1179
C. jeikeium (R)
PF-191 S. epidermidis (A) QFCNFAWLFLASNNAQVSALA 1180
MRSA (H)
C. jeikeium (R)
PF-192 S. epidermidis (D) VEEDEAPPPHY 1181
PF-196 S. epidermidis (C) TTARYIRRQCHTSITPLSQG 1182
C. jeikeium (R)
PF-199 S. epidermidis (C) FPAFSFGAIAGSVSVAR 1183
M. luteus (A)
C. jeikeium (R)
PF-203 S. epidermidis (A) SWKCHHLAI 1184
C. jeikeium (R)
PF-204 S. epidermidis (C) ALQKQDMNLPSVKNQLVFLKSTG 1185
M. luteus (C)
P. aeruginosa (H)
C. jeikeium (D)
PF-208 S. epidermidis (D) DAYHCHLVRSPDAHDLSMRIGFV 1186
C. jeikeium (A)
PF-209 S. epidermidis (C) NYAVVSHT 1187
P. aeruginosa (H)
MRSA (I)
PF-212 M. luteus (M) NDSKASN 1188
PF-215 M. luteus (T) ELKITNYNVNTVLYRYYKWGNDLCE 1189
PF-220 S. pneumoniae (H) VDPADDGTRHIRPEDGDPIEIDE 1190
PF-224 M. luteus (T) DYFYITLSQKNTF 1191
PF-226 S. epidermidis (C) LMFFSENMDKRDTLSGKFRYFAGSKVI 1192
M. luteus (T) KLMNWLSENGK
PF-233 S. epidermidis (C) DANAMARTTIAIVYILALIALTISYSL 1193
PF-234 M. luteus (T) RTPYILRS 1194
PF-235 M. luteus (T) GIPFSKPHKRQVNYMKSDVLAYIEQNK 1195
MAHTA
PF-249 M. luteus (R) INSRYKISF 1196
PF-250 M. luteus (T) SEDIFGRLANEKANGLEELRKIRLKQ 1197
PF-255 M. luteus (M) DHKINESQHNPFRSDSNKQNVDFF 1198
PF-257 M. luteus (R) VWENRKKYLENEIERHNVFLKLGQEVI 1199
KGLNALASRGR
PF-264 M. luteus (H) MQSLSNRQSLIASYILMGIFLSFGYPPA 1200
SLSKFFCRLSHL
PF-270 M. luteus (H) MYLTPYAWIAVGSIFAFSVTTIKIGDQN 1201
DEKQKSHKNDVHKR
PF-271 M. luteus (T) AAQPQTTSP 1202
PF-273 S. epidermidis (C) LVGALLIFVALIYMVLKGNADKN 1203
PF-274 M. luteus (M) SIQEAEKIIKNDPFYIHDVADYDFMWF 1204
EPSKSLEEIKEFV
PF-276 M. luteus (M) LDLALSTNSLNLEGFSF 1205
PF-278 S. epidermidis (I) LSLATFAKIFMTRSNWSLKRFNRL 1206
M. luteus (R)
C. albicans (B)
PF-283 S. epidermidis (H) MIRIRSPTKKKLNRNSISDWKSNTSGRF 1207
B. subtilis (H) FY
PF-289 B. subtilis (C) MGRHLWNPSYFVATVSENTEEQIRKY 1208
RKNK
PF-290 S. epidermidis (C) MVHDMTNGTLIIVKH 1209
PF-292 S. epidermidis (C) SFVSTTVRLIFEESKRYKF 1210
B. subtilis (C)
PF-293 S. epidermidis (C) YDPLK 1211
PF-294 S. epidermidis (C) DFLVNFLWFKGELNWGKKRYK 1212
PF-296 S. epidermidis (C) GAFGMPSIKTNTICGEKGKFISACDAW 1213
B. subtilis (C) LSNLK
PF-297 S. epidermidis (C) ISKGIDDIVYVINKILSIGNIFKIIKRK 1214
B. subtilis (C)
PF-301 S. epidermidis (C) GIVLIGLKLIPLLANVLN 1215
B. subtilis (C)
PF-303 B. subtilis (C) EYPWSWISEPWPWDKSFYK 1216
PF-305 B. subtilis (C) MREWICPSCNETHDRDINASINILKEGL 1217
RLITIQNK
PF-306 B. subtilis (C) GCILPHKKDNYNYIMSKFQDLVKITSKK 1218
PF-307 S. epidermidis (T) MKRRRCNWCGKLFYLEEKSKEAYCC 1219
B. subtilis (H) KECRKKAKKVKK
C. albicans (B)
PF-310 S. epidermidis (C) GVALIGTILVPLLSGLFG 1220
PF-313 S. epidermidis (C) YITSHKNARAIIKKFERDEILEEVITHYL 1221
NRK
PF-318 S. epidermidis (C) MGRHLWNPSYFVATVSENTEEQIRKYI 1222
B. subtilis (C) NNQKKQVK
PF-319 S. epidermidis (C) SIGSMIGMYSFRHKTKHIKFTFGIPFILF 1223
B. subtilis (C) LQFLLVYFYILK
PF-322 S. epidermidis (C) GIVLIGLKLIPLLANVLR 1224
B. subtilis (H)
PF-335 S. epidermidis (C) AAYPIEDWSDWYEDFFIMLSNI 1225
B. subtilis (C)
PF-339 S. epidermidis (C) KKIDILINKYMYLSK 1226
B. subtilis (C)
PF-342 S. epidermidis (C) AFSGVYKTLIVYTRRK 1227
B. subtilis (C)
PF-344 E. coli (A) DERLPEAKAIRNFNGSVMVLGR 1228
PF-347 S. epidermidis (C) GIFTGVTVVVSLKHC 1229
E. coli (C)
MRSA (C)
E. faecalis (C)
PF-349 S. epidermidis (C) MPKSCHVPVLCDFFFLVIIKFLALFKTI 1230
E. coli (C) QS
MRSA (C)
E. faecalis (C)
PF-350 S. epidermidis (C) LAVILRAIVY 1231
E. coli (C)
MRSA (C)
PF-354 MRSA (H) FTFSKCRASNGRGFGTLWL 1232
PF-355 S. epidermidis (C) WIAIGLLLYFSLKNQ 1233
E. coli (C)
P. aeruginosa (A)
MRSA (A)
S. pneumoniae (D)
E. faecalis (D)
C. jejuni (D)
PF-356 S. epidermidis (S) VSIKIGAIVIGMIGLMELLTE 1234
P. aeruginosa (A)
MRSA (C)
S. pneumoniae (R)
E. faecalis (R)
C. jejuni (D)
PF-357 S. epidermidis (M) MLTIIIGFIFWTMTLMLGYLIGEREGRK 1235
M. luteus (C) HE
MRSA (M)
S. pneumoniae (M)
PF-360 S. epidermidis (S) MEQKVKVIFVPRSKPDNQLKTFVSAVL 1236
E. coli (C) FKA
MRSA (H)
PF-362 E. coli (C) NIERILKEKVWMIRCVE 1237
MRSA (C)
PF-363 S. epidermidis (S) SMLSVTVMCLMHASVAANQAMEKKV 1238
E. coli (C)
MRSA (H)
S. pneumoniae (R)
E. faecalis (D)
C. jejuni (D)
PF-366 S. epidermidis (R) ALCSVIKAIELGIINVHLQ 1239
E. coli (C)
P. aeruginosa (A)
MRSA (D)
S. pneumoniae (C)
E. faecalis (C)
C. jejuni (D)
PF-369 S. epidermidis (S) MSEAVNLLRGARYSQRYAKNQVPYEV 1240
E. coli (R) IIEK
MRSA (H)
E. faecalis (C)
PF-370 S. epidermidis (C) VIFLHKESGNLKEIFY 1241
E. coli (R)
MRSA (C)
PF-373 S. epidermidis (M) HFYLLFER 1242
MRSA (M)
PF-374 S. epidermidis (C) HLFFVKGMFILCQKNQINDE 1243
E. coli (C)
MRSA (M)
E. faecalis (C)
PF-375 S. epidermidis (C) MDSAKAQTMRTDWLAVSCLVASAYL 1244
E. coli (C) RSMLA
MRSA (C)
E. faecalis (C)
PF-376 S. epidermidis (C) MTVFEALMLAIAFATLIVKISNKNDKK 1245
E. coli (C)
MRSA (C)
E. faecalis (C)
PF-378 S. epidermidis (M) ESAKSNLNFLMQEEWALFLLL 1246
MRSA (M)
PF-379 S. epidermidis (C) VFVVLFIIYLASKLLTKLFPIKK 1247
E. coli (C)
MRSA (C)
E. faecalis (C)
PF-380 S. epidermidis (C) KKIIPLITLFVVTLVG 1248
E. coli (C)
P. aeruginosa (A)
MRSA (D)
S. pneumoniae (D)
E. faecalis (C)
C. jejuni (D)
PF-381 S. epidermidis (C) QGANPCQQVGFTVNDPDCRLAKTV 1249
E. coli (R)
MRSA (C)
E. faecalis (C)
PF-382 MRSA (M) KYKCSWCKRVYTLRKDHKTAR 1250
PF-383 S. epidermidis (C) WSEIEINTKQSN 1251
E. coli (R)
PF-385 E. coli (A) MIKKSILKIKYYVPVLISLTLILSA 1252
PF-386 S. epidermidis (C) FTLTLITTIVAILNYKDKKK 1253
E. coli (C)
MRSA (C)
E. faecalis (C)
PF-387 S. epidermidis (C) GAVGIAFFAGNMKQDKRIADRQNKKS 1254
E. coli (M) EKK
MRSA (C)
E. faecalis (C)
PF-389 S. epidermidis (R) GLQFKEIAEEFHITTTALQQWHKDNGY 1255
MRSA (C) PIYNKNNRK
S. pneumoniae (D)
E. faecalis (R)
C. jejuni (R)
PF-390 S. epidermidis (D) VVAYVITQVGAIRF 1256
E. coli (C)
MRSA (D)
S. pneumoniae (D)
E. faecalis (D)
C. jejuni (D)
PF-392 MRSA (S) DPAGCNDIVRKYCK 1257
E. faecalis (A)
C. jejuni (A)
PF-393 S. epidermidis (R) DLVQSILSEFKKSG 1258
MRSA (C)
S. pneumoniae (R)
E. faecalis (A)
C. jejuni (R)
PF-394 MRSA (C) VLKEECYQKN 1259
E. faecalis (A)
PF-395 S. epidermidis (C) YCVPLGNMGNMNNKIW 1260
E. coli (R)
MRSA (C)
PF-396 S. epidermidis (S) LIYTILASLGVLTVLQAILGREPKAVKA 1261
E. coli (C)
MRSA (C)
E. faecalis (C)
PF-397 S. epidermidis (C) VEDLMEDLNA 1262
PF-398 S. epidermidis (C) ILVVLAGILLVVLSYVGISKFKMNC 1263
E. coli (C)
MRSA (C)
E. faecalis (C)
PF-399 S. epidermidis (C) FPIISALLGAIICIAIYSFIVNRKA 1264
E. coli (C)
MRSA (C)
E. faecalis (C)
PF-401 S. epidermidis (C) YWLSRVTTGHSFAFEKPVPLSLTIK 1265
E. coli (R)
MRSA (C)
E. faecalis (C)
PF-403 S. epidermidis (M) LLSTEQLLKYYDGETFDGFQLPSNE 1266
E. coli (R)
MRSA (M)
PF-404 S. epidermidis (M) VLYFQATVV 1267
MRSA (M)
PF-405 MRSA (M) LVRIEVDDLEEWYERNFI 1268
PF-406 S. epidermidis (C) YLEMNADYLSNMDIFDELWEKYLENNK 1269
MRSA (M)
PF-407 S. epidermidis (M) KPKNKKEKTVISYEKLLSMY 1270
MRSA (C)
S. pneumoniae (R)
E. faecalis (R)
PF-408 S. epidermidis (M) YCVPLGNMGNMNNKIW 1271
MRSA (M)
PF-410 S. epidermidis (C) FALELIALCRNLFIVYFP 1272
E. coli (S)
MRSA (M)
E. faecalis (C)
PF-411 S. epidermidis (C) WVAVAILLNIALQTQLT 1273
E. coli (C)
P. aeruginosa (A)
MRSA (D)
S. pneumoniae (D)
E. faecalis (D)
C. jejuni (D)
PF-413 S. epidermidis (C) TFAGSIKIGVPDLVHVTFNCKR 1274
E. coli (S)
MRSA (C)
PF-414 S. pneumoniae (H) LLNKKLE 1275
PF-415 S. pneumoniae (D) MIDVTIGQKSKTGAFNASYSICFSGENF 1276
SF
PF-416 S. pneumoniae (H) SKAGLYGKIERSDKRE 1277
PF-417 S. epidermidis (M) DSYFRS 1278
MRSA (M)
S. pneumoniae (M)
PF-418 S. epidermidis (M) FFLVHFYIRKRKGKVSIFLNYF 1279
E. coli (C)
MRSA (D)
S. pneumoniae (D)
E. faecalis (D)
C. jejuni (D)
PF-419 S. pneumoniae (H) VVTGKVGSLPQIK 1280
PF-421 S. pneumoniae (H) KHCFEITDKTDVV 1281
PF-422 S. epidermidis (R) MSRKKYENDEKSQKKLKIGRKSDVFY 1282
MRSA (C) GIID
S. pneumoniae (C)
E. faecalis (R)
C. jejuni (R)
PF-423 S. pneumoniae (H) AGKKERLLSFREQFLNKNKKK 1283
PF-424 S. pneumoniae (H) IAAFVTSRAFSDTVSPI 1284
PF-425 S. epidermidis (D) MMELVLKTIIGPIVVGVVLRIVDKWLN 1285
E. coli (C) KDK
P. aeruginosa (A)
C. albicans (A)
MRSA (D)
S. pneumoniae (D)
E. faecalis (D)
C. jejuni (D)
PF-426 S. epidermidis (D) MLQKYTQMISVTKCIITKNKKTQENVD 1286
E. coli (C) AYN
C. albicans (A)
MRSA (D)
S. pneumoniae (D)
E. faecalis (D)
C. jejuni (D)
PF-427 E. coli (C) YVLEYHGLRATQDVDAFMAL 1287
MRSA (C)
S. pneumoniae (R)
E. faecalis (C)
PF-428 S. pneumoniae (H) ENEESIF 1288
PF-429 S. epidermidis (C) AATLICVGSGIMSSL 1289
MRSA (C)
S. pneumoniae (M)
E. faecalis (C)
PF-430 S. epidermidis (M) AVVCGYLAYTATS 1290
MRSA (M)
S. pneumoniae (M)
PF-431 S. epidermidis (M) VAYAAICWW 1291
MRSA (C)
S. pneumoniae (R)
E. faecalis (R)
C. jejuni (R)
PF-432 S. epidermidis (M) FNGDSEFFLCIAF 1292
E. coli (R)
P. aeruginosa (A)
MRSA (M)
S. pneumoniae (D)
E. faecalis (D)
C. jejuni (D)
PF-433 S. pneumoniae (H) MRKEFHNVLSSGQLLADKRPARDYNRK 1293
PF-434 S. pneumoniae (S) GQLLADKRPARDYNRK 1294
PF-437 S. pneumoniae (I) FQKPFTGEEVEDFQDDDEIPTII 1295
PF-439 S. epidermidis (C) RVLVLKKFHGIMDGNRNVAVFFVGQ 1296
E. coli (R)
MRSA (M)
S. pneumoniae (R)
E. faecalis (C)
PF-440 S. epidermidis (C) MFIISPDLFNIAVILYILFFIHDILLLILS 1297
E. coli (R)
MRSA (C)
S. pneumoniae (R)
E. faecalis (C)
PF-442 MRSA (M) MQIFYIKTKIFLSFFLFLLIFSQCFYKIEE 1298
S. pneumoniae (C)
PF-443 E. coli (R) KLLYFFNYFENLQQVHLLVQL 1299
MRSA (C)
S. pneumoniae (C)
PF-444 S. epidermidis (C) MAAKLWEEGKMVYASSASMTKRLKL 1300
E. coli (R) AMSKV
MRSA (C)
S. pneumoniae (R)
E. faecalis (C)
PF-445 S. pneumoniae (M) ASMTKRLKLAMSKV 1301
PF-446 S. pneumoniae (H) SGNEKV 1302
PF-447 S. epidermidis (C) IDKSRNKDQFSHIFGLYNICSG 1303
MRSA (C)
S. pneumoniae (C)
E. faecalis (C)
PF-448 S. pneumoniae (I) SLQSQLGPCLHDQRH 1304
PF-449 S. pneumoniae (H) MPTTKSKQKGWTNTKKASNTQ 1305
PF-450 MRSA (C) HRNLIILQRTIFI 1306
S. pneumoniae (C)
E. faecalis (C)
PF-451 S. epidermidis (C) MVNYIIGSYMLYREQNNNEALRKFDIT 1307
E. coli (R) LAM
MRSA (C)
S. pneumoniae (C)
E. faecalis (C)
PF-452 S. epidermidis (C) MNNWIKVAQISVTVINEVIDIMKEKQN 1308
E. coli (C) GGK
MRSA (C)
S. pneumoniae (R)
E. faecalis (C)
PF-453 S. epidermidis (C) IIQDIAHAFGY 1309
E. coli (C)
MRSA (C)
S. pneumoniae (C)
PF-454 S. epidermidis (C) MSVFVPVTNIFMFIMSPIFNVNLLHFKV 1310
E. coli (R) YI
P. aeruginosa (H)
MRSA (C)
S. pneumoniae (R)
E. faecalis (C)
PF-455 S. pneumoniae (A) MARNDDDIKKIKGTLGQSPEVYGERK 1311
LPYT
PF-456 E. faecalis (A) TCVKPRTIN 1312
C. jejuni (A)
PF-457 S. pneumoniae (M) INKYHHIA 1313
PF-458 P. aeruginosa (H) ISLIIFIMLFVVALFKCITNYKHQS 1314
MRSA (M)
S. pneumoniae (M)
PF-459 S. pneumoniae (H) EKRMSFNENQSHRPLL 1315
PF-460 S. epidermidis (C) MEHVLPFQNTPPNIVIIYKDFTHLKSITFS 1316
E. coli (H)
MRSA (C)
S. pneumoniae (R)
E. faecalis (C)
PF-461 MRSA (R) MTLAIKNCSVTKCLGFGDFVNDDSDS 1317
S. pneumoniae (R) YFDA
E. faecalis (A)
PF-462 S. pneumoniae (H) KNKTDTL 1318
PF-464 S. pneumoniae (S) VDMVNRFLGN 1319
PF-465 S. pneumoniae (H) KPVGKALEEIADGKIEPVVPKEYLG 1320
PF-466 S. pneumoniae (H) VRKSDQ 1321
PF-467 S. pneumoniae (H) YYKDYFKEI 1322
PF-468 S. pneumoniae (H) EDNKDKKDKKDK 1323
PF-469 S. epidermidis (D) YKVNYNNIDNHFNTLRH 1324
E. coli (C)
MRSA (D)
S. pneumoniae (D)
E. faecalis (D)
C. jejuni (D)
PF-470 E. faecalis (A) PYSDSYATRPHWEQHRAR 1325
C. jejuni (A)
PF-471 S. epidermidis (C) MVGKIRGVTPRNDLLNANITGQLNLN 1326
E. coli (C) YRLI
P. aeruginosa (A)
MRSA (D)
S. pneumoniae (D)
E. faecalis (C)
C. jejuni (D)
PF-472 MRSA (C) MHISHLLDEVEQTEREKAVNVLENMN 1327
S. pneumoniae (R) GNVI
E. faecalis (A)
C. jejuni (R)
PF-473 S. epidermidis (R) MAADIISTIGDLVKWIIDTVNKFKK 1328
E. coli (C)
MRSA (C)
S. pneumoniae (H)
E. faecalis (R)
C. jejuni (R)
PF-474 S. epidermidis (C) MHRNLVLVKMEPIPHIMIIANQIGIIIEKA 1329
E. coli (C)
P. aeruginosa (A)
C. albicans (B)
MRSA (D)
S. pneumoniae (D)
E. faecalis (C)
C. jejuni (D)
PF-475 S. epidermidis (M) MREKVRFTQAFKLFWTNYFNFKGRSR 1330
C. albicans (B) RSEY
MRSA (S)
S. pneumoniae (R)
E. faecalis (R)
C. jejuni (R)
PF-476 S. pneumoniae (H) WADAQYKLCENCSE 1331
PF-477 S. pneumoniae (H) HKNKLNIPHIKS 1332
PF-478 S. epidermidis (C) HLFILKSHLKPFPPFRYTYD 1333
E. coli (C)
MRSA (H)
S. pneumoniae (C)
PF-479 S. pneumoniae (C) AYILKRREEKNK 1334
PF-480 S. epidermidis (C) MVEILVNTAISVYIVALYTQWLSTRDN 1335
E. coli (R) LKA
MRSA (C)
S. pneumoniae (R)
E. faecalis (C)
PF-482 S. pneumoniae (S) LVGYVRTSGTVRSYKIN 1336
PF-484 E. faecalis (A) HKKDIRKQVFKN 1337
PF-485 S. pneumoniae (A) KNSMSRSIALID 1338
PF-511 S. pneumoniae (H) VMQSLYVKPPLILVTKLAQQN 1339
PF-512 S. pneumoniae (H) SFMPEIQKNTIPTQMK 1340
PF-513 S. pneumoniae (M) SNGVGLGVGIGSGIRF-NH2 1341
PF-514 S. epidermidis (C) QRFYKLFYHIDLTNEQALKLFQVK 1342
E. coli (R)
S. pneumoniae (M)
E. faecalis (C)
PF-515 S. pneumoniae (H) DKSTQDKDIKQAKLLAQELGL-NH2 1343
PF-516 S. pneumoniae (H) ASKQASKQASKQASKQ 1344
PF-517 S. pneumoniae (M) VKPTMTASLISTVC 1345
PF-518 S. epidermidis (C) SFYSKYSRYIDNLAGAIFLFF 1346
E. coli (R)
MRSA (C)
S. pneumoniae (M)
E. faecalis (C)
PF-519 E. coli (R) YLVYSGVLATAAAF-NH2 1347
MRSA (C)
S. pneumoniae (S)
E. faecalis (C)
PF-520 S. pneumoniae (M) LGLTAGVAYAAQPTNQPTNQPTNQPT 1348
NQPTNQPTNQPRW-NH2
PF-521 S. pneumoniae (H) CGKLLEQKNFFLKTR 1349
PF-522 S. pneumoniae (H) FELVDWLETNLGKILKSKSA-NH2 1350
PF-524 E. coli (M) PDAPRTCYHKPILAALSRIVVTDR 1351
MRSA (C)
S. pneumoniae (M)
E. faecalis (C)
PF-525 S. pneumoniae (H) KFSDQIDKGQDALKDKLGDL 1352
PF-526 S. epidermidis (C) VLLLFIFQPFQKQLL-NH2 1353
E. coli (R)
C. albicans (C)
MRSA (C)
S. pneumoniae (R)
PF-527 S. epidermidis (M) GSVIKKRRKRMAKKKHRKLLKKTRIQ 1354
M. luteus (S) RRRAGK
B. subtilis (I)
P. aeruginosa (I)
C. albicans (B)
MRSA (I)
S. pneumoniae (H)
C. jeikeium (I)
C. jejuni (M)
PF-528 S. epidermidis (H) LVDVVVLIRRHLPKSCS-NH2 1355
E. coli (H)
C. albicans (C)
MRSA (H)
S. pneumoniae (R)
PF-529 S. pneumoniae (H) LSEMERRRLRKRA-NH2 1356
PF-530 S. epidermidis (H) SKFKVLRKIIIKEYKGELMLSIQKQR 1357
E. coli (R)
MRSA (C)
S. pneumoniae (R)
E. faecalis (C)
PF-531 S. epidermidis (I) YIQFHLNQQPRPKVKKIKIFL-NH2 1358
E. coli (M)
P. aeruginosa (I)
S. pneumoniae (C)
PF-532 E. coli (C) KFIYKYKLSFIIYKILIQTLTMELNK 1359
MRSA (C)
S. pneumoniae (C)
E. faecalis (C)
PF-533 S. epidermidis (H) KTPNDKIHKTIIIKHIIL 1360
E. coli (R)
MRSA (H)
S. pneumoniae (C)
E. faecalis (C)
PF-534 S. epidermidis (C) KYFHLFYHNIIHYSKQHLSLKVDFKN- 1361
E. coli (R) NH2
MRSA (C)
S. pneumoniae (R)
E. faecalis (C)
PF-535 P. aeruginosa (H) NIKTRKRALKIIKQHQRSK 1362
S. pneumoniae (H)
PF-536 S. epidermidis (C) MEPIPHIMIIANQIGIIIEKA 1363
E. coli (R)
P. aeruginosa (H)
MRSA (C)
S. pneumoniae (M)
E. faecalis (C)
PF-537 S. pneumoniae (C) LANDYYKKTKKSW 1364
PF-538 S. pneumoniae (H) KNKKQTDILEKVKEILDKKKKTKSVG 1365
QKLY
PF-539 MRSA (H) SIILTKKKRRKIPLSIDSQIYKYTFKQ 1366
S. pneumoniae (A)
PF-540 S. epidermidis (H) KSILILIKVIFIGQTTIIL 1367
E. coli (R)
MRSA (H)
S. pneumoniae (R)
PF-541 E. coli (H) RRNLNSPNIKTRKRALKIIKQHQRSK 1368
S. pneumoniae (H)
PF-542 S. pneumoniae (H) KKDNPSLNDQDKNAVLNLLALAK 1369
PF-543 S. mutans (S) NILFGIIGFVVAMTAAVIVTAISIAK 1370
S. epidermidis (D)
M. luteus (C)
E. coli (C)
MRSA (D)
S. pneumoniae (D)
PF-544 S. epidermidis (D) FGEKQMRSWWKVHWFHP 1371
MRSA (D)
S. pneumoniae (M)
E. faecalis (R)
PF-545 B. subtilis (I) RESKLIAMADMIRRRI-NH2 1372
C. albicans (B)
E. faecalis (H)
C. jeikeium (H)
PF-546 S. epidermidis (D) PIIAPTIKTQIQ 1373
E. coli (R)
MRSA (D)
S. pneumoniae (D)
E. faecalis (D)
C. jeikeium (D)
PF-547 S. epidermidis (R) WSRVPGHSDTGWKVWHRW-NH2 1374
B. subtilis (I)
MRSA (M)
E. faecalis (R)
PF-548 S. epidermidis (M) ARPIADLIHFNSTTVTASGDVYYGPG 1375
M. luteus (A)
B. subtilis (C)
MRSA (M)
S. pneumoniae (D)
C. jeikeium (R)
C. jejuni (D)
PF-549 B. subtilis (D) TGIGPIARPIEHGLDS 1376
MRSA (C)
PF-550 B. subtilis (D) STENGWQEFESYADVGVDPRRYVPL 1377
PF-551 MRSA (C) QVKEKRREIELQFRDAEKKLEASVQAE 1378
PF-552 B. subtilis (D) ELDKADAALGPAKNLAPLDVINRS 1379
PF-553 B. subtilis (D) LTIVGNALQQKNQKLLLNQKKITSLG 1380
MRSA (M)
S. pneumoniae (R)
C. jeikeium (R)
PF-554 B. subtilis (D) AKNFLTRTAEEIGEQAVREGNINGP 1381
PF-555 MRSA (M) EAYMRFLDREMEGLTAAYNVKLFTEA 1382
S. pneumoniae (R) IS
C. jejuni (R)
PF-556 S. epidermidis (A) SLQIRMNTLTAAKASIEAA 1383
M. luteus (A)
B. subtilis (C)
MRSA (M)
S. pneumoniae (D)
E. faecalis (A)
C. jeikeium (D)
C. jejuni (R)
PF-557 B. subtilis (D) AANKAREQAAAEAKRKAEEQAR 1384
PF-558 S. epidermidis (M) ADAPPPLIVRYS 1385
B. subtilis (D)
MRSA (C)
S. pneumoniae (R)
C. jejuni (H)
PF-559 B. subtilis (C) SRPGKPGGVSIDVSRDRQDILSNYP 1386
C. jejuni (A)
PF-560 B. subtilis (D) FGNPFRGFTLAMEADFKKRK 1387
MRSA (C)
S. pneumoniae (R)
C. jejuni (A)
PF-561 B. subtilis (D) ESLEADVQAELDTEAAKYPALPASF 1388
MRSA (M)
PF-562 S. epidermidis (A) TPEQWLERSTVVVTGLLNRK 1389
M. luteus (R)
MRSA (M)
S. pneumoniae (D)
C. jejuni (R)
PF-563 B. subtilis (D) RPELDNELDVVQNSASLDKLQASYN 1390
S. pneumoniae (H)
C. jejuni (H)
PF-564 B. subtilis (D) TIILNDQINSLQERLNKLNAETDRR 1391
MRSA (C)
C. jeikeium (R)
C. jejuni (R)
PF-565 B. subtilis (D) RAEAEAQRQAEADAKRKAEEAARL 1392
MRSA (C)
PF-566 M. luteus (D) EAQQVTQQLGADFNAITTPTATKV 1393
B. subtilis (C)
MRSA (M)
S. pneumoniae (D)
C. jeikeium (C)
C. jejuni (D)
PF-567 M. luteus (C) QQRVKAVDASLSQVSTQVSGAVASA 1394
MRSA (D)
S. pneumoniae (D)
C. jeikeium (C)
C. jejuni (D)
PF-569 B. subtilis (D) KSKISEYTEKEFLEFVEDIYTNNK 1395
PF-571 B. subtilis (D) SDLLYYPNENREDSPAGVVKEVKE 1396
PF-572 B. subtilis (D) WRASKGLPGFKAG 1397
S. pneumoniae (R)
PF-573 S. pneumoniae (C) EKKLIVKLIDSIGKSHEEIVGAG 1398
PF-574 B. subtilis (D) LVKSGKLESPYEHSEHLTLSQEKGLE 1399
PF-575 P. aeruginosa (A) LNFRAENKILEKIHISLIDTVEGSA 1400
S. pneumoniae (A)
C. jeikeium (A)
C. jejuni (R)
PF-576 S. epidermidis (A) AYSGELPEPLVRKMSKEQVRSVMGK 1401
E. coli (A)
MRSA (R)
S. pneumoniae (C)
C. jejuni (C)
PF-577 S. epidermidis (A) PFETRESFRVPVIGILGGWDYFMHP 1402
E. coli (A)
P. aeruginosa (A)
MRSA (M)
S. pneumoniae (R)
E. faecalis (A)
C. jejuni (R)
PF-578 S. mutans (D) QKANLRIGFTYTSDSNVCNLTFALLGSK 1403
S. epidermidis (D)
M. luteus (C)
P. mirabilis (C)
E. coli (C)
MRSA (C)
S. pneumoniae (D)
PF-580 S. epidermidis (M) EILNNNQVIKELTMKYKTQFESNLGG 1404
M. luteus (C) WTARARR
MRSA (M)
S. pneumoniae (C)
PF-581 MRSA (A) WTARARR 1405
S. pneumoniae (A)
E. faecalis (A)
C. jejuni (A)
PF-582 E. faecalis (A) NLKTIEKECPFCNNKMDIKLKD 1406
PF-583 S. mutans (F) KFQGEFTNIGQSYIVSASHMSTSLNTGK 1407
S. epidermidis (I)
MRSA (I)
S. pneumoniae (D)
PF-584 S. epidermidis (C) SYIKNLSNQKFLIAF 1408
E. coli (C)
MRSA (D)
S. pneumoniae (D)
E. faecalis (D)
C. jejuni (D)
PF-585 S. epidermidis (S) DYNHLLNVVQDWVNTN 1409
MRSA (S)
S. pneumoniae (R)
E. faecalis (A)
C. jejuni (R)
PF-586 S. epidermidis (C) FFNQANYFFKEF 1410
E. coli (C)
MRSA (D)
S. pneumoniae (D)
E. faecalis (D)
C. jejuni (D)
PF-587 S. pneumoniae (C) ASGKYQSYLLNVYVDSKKDRLDIFDK 1411
LKAKAKFVL
PF-588 E. faecalis (A) ESVEAIKAKAIK 1412
PF-589 MRSA (M) APLRIDEIRNSNVIDEVLDCAPKKQEHF 1413
S. pneumoniae (C) FVVPKIIE
PF-590 C. jejuni (R) YYQAKLFPLL 1414
PF-591 S. pneumoniae (R) DLLKSLLGQDGAKNDEIIEFIKIIMEK 1415
E. faecalis (A)
C. jejuni (C)
PF-592 S. epidermidis (M) IMKNYKYFKLFIVKYALF 1416
E. coli (C)
MRSA (D)
S. pneumoniae (D)
E. faecalis (D)
C. jejuni (S)
PF-593 E. faecalis (A) MEISTLKKEKLHVKDELSQYLANYKK 1417
PF-594 E. faecalis (C) IVSAIV 1418
PF-595 S. epidermidis (C) LQNKIYELLYIKERSKLCS 1419
E. coli (C)
MRSA (D)
S. pneumoniae (R)
E. faecalis (D)
C. jejuni (D)
PF-596 S. epidermidis (D) SKMWDKILTILILILELIRELIKL 1420
E. coli (C)
MRSA (D)
S. pneumoniae (D)
E. faecalis (D)
C. jejuni (D)
PF-597 E. faecalis (A) DEIKVSDEEIEKFIKENNL 1421
PF-598 S. epidermidis (R) MKFMLEVRNKAISAYKEITRTQI 1422
E. coli (C)
MRSA (D)
S. pneumoniae (R)
E. faecalis (R)
C. jejuni (R)
PF-599 S. epidermidis (M) LFEIFKPKH 1423
MRSA (C)
S. pneumoniae (R)
E. faecalis (A)
C. jejuni (R)
PF-600 S. mutans (S) TKKIELKRFVDAFVKKSYENYILEREL 1424
S. epidermidis (C) KKLIKAINEELPTK
M. luteus (C)
E. coli (H)
MRSA (M)
S. pneumoniae (R)
PF-601 E. faecalis (A) YRVTVKALE 1425
C. jejuni (A)
PF-602 E. faecalis (A) LEKEKKEYIEKLFKTK 1426
PF-603 S. epidermidis (D) IDKLKKMNLQKLSYEVRISQDGKSIYA 1427
M. luteus (A) RIK
E. coli (M)
MRSA (M)
S. pneumoniae (C)
PF-604 E. faecalis (A) LMEQVEV 1428
PF-605 S. epidermidis (R) HYRWNTQWWKY 1429
E. coli (C)
P. aeruginosa (A)
C. albicans (B)
MRSA (C)
S. pneumoniae (D)
E. faecalis (R)
C. jejuni (R)
PF-606 S. mutans (I) FESKILNASKELDKEKKVNTALSFNSH 1430
S. epidermidis (I) QDFAKAYQNGKI
C. albicans (B)
MRSA (I)
S. pneumoniae (H)
PF-607 S. epidermidis (M) YIESDPRKFDYIFGAIRDH 1431
MRSA (S)
S. pneumoniae (R)
E. faecalis (A)
C. jejuni (R)
PF-609 MRSA (C) TEIKLDNNEYLVLNLDDILGILK 1432
S. pneumoniae (R)
E. faecalis (A)
C. jejuni (R)
PF-610 S. epidermidis (C) VFLKLKTSKIDLASIIFYP 1433
E. coli (C)
MRSA (D)
S. pneumoniae (D)
E. faecalis (D)
C. jejuni (D)
PF-612 S. mutans (F) GTTLKYGLERQLKIDIHPEITIINLNGGA 1434
S. epidermidis (C) DEFAKL
M. luteus (A)
P. mirabilis (C)
E. coli (C)
MRSA (C)
S. pneumoniae (C)
PF-613 S. epidermidis (R) ADEFAKL 1435
MRSA (C)
E. faecalis (A)
PF-614 S. epidermidis (M) GLDIYA 1436
S. pneumoniae (R)
E. faecalis (A)
C. jejuni (R)
PF-615 S. epidermidis (D) FLNRFIFYIFTVKTKSALIKNLFLD 1437
E. coli (C)
MRSA (D)
S. pneumoniae (D)
E. faecalis (D)
C. jejuni (D)
PF-616 S. epidermidis (R) IVFVVTKEKK 1438
E. faecalis (A)
PF-617 C. albicans (H) PMNAAEPE 1439
S. pneumoniae (I)
E. faecalis (H)
PF-618 S. pneumoniae (I) KLNTLNKKDNPSLNDQDKNAVLNLLA 1440
E. faecalis (H) LAK
PF-619 S. epidermidis (M) WSRVPGHSDTGWKVWHRW 1441
E. coli (C)
MRSA (M)
S. pneumoniae (C)
PF-621 S. pneumoniae (I) PPSSFLV 1442
E. faecalis (H)
PF-622 S. epidermidis (D) TREDVFSVRLINNIVNKQA 1443
MRSA (D)
S. pneumoniae (M)
E. faecalis (D)
C. jeikeium (D)
PF-623 S. epidermidis (M) VLFAVYLGALDWLFSWLTQKM 1444
MRSA (D)
S. pneumoniae (D)
E. faecalis (D)
C. jeikeium (R)
PF-624 S. mutans (D) VFLLDSYCFVKINL 1445
S. epidermidis (D)
M. luteus (C)
P. mirabilis (C)
E. coli (C)
MRSA (C)
S. pneumoniae (D)
PF-625 S. pneumoniae (H) SDSTNNARTRKKARDVTTKDIDK 1446
PF-626 S. pneumoniae (H) KYDFDDFEPEEA 1447
PF-627 S. epidermidis (H) INDLLSYFTLHEK 1448
C. albicans (B)
MRSA (R)
S. pneumoniae (I)
E. faecalis (H)
PF-629 S. epidermidis (C) GLAAIATVFALY 1449
MRSA (D)
S. pneumoniae (M)
E. faecalis (R)
C. jeikeium (R)
PF-630 MRSA (M) IPATPIIHS 1450
PF-631 S. pneumoniae (I) LIIYFSKTGNTARATRQI 1451
E. faecalis (H)
PF-632 S. epidermidis (D) TTIQGVASLEKHGFRYTIIYPTRI 1452
B. subtilis (H)
C. albicans (B)
MRSA (D)
S. pneumoniae (M)
E. faecalis (D)
C. jeikeium (D)
PF-634 S. mutans (D) MPKARPVNHNKKKSKITIKSNFTLFYM 1453
S. epidermidis (D) FNP
M. luteus (C)
P. mirabilis (C)
E. coli (C)
MRSA (D)
S. pneumoniae (D)
PF-635 S. epidermidis (M) MNAHGHSLIFQKMIVHAFAFFSKQKN 1454
C. albicans (B) YLYF
MRSA (D)
S. pneumoniae (D)
E. faecalis (D)
C. jeikeium (D)
PF-636 B. subtilis (H) LVRLA 1455
C. albicans (B)
S. pneumoniae (H)
E. faecalis (H)
PF-637 S. epidermidis (M) SRIKQDARSVRKYDRIGIFFYSFKSA 1456
MRSA (M)
S. pneumoniae (M)
E. faecalis (D)
C. jeikeium (D)
PF-638 S. epidermidis (R) TFILPK 1457
MRSA (M)
S. pneumoniae (I)
E. faecalis (H)
PF-639 C. albicans (B) QATQIKSWIDRLLVSED 1458
MRSA (R)
S. pneumoniae (I)
E. faecalis (H)
PF-640 C. albicans (B) MGDINRNF 1459
S. pneumoniae (I)
E. faecalis (H)
PF-642 MRSA (M) FTTPMIGIPAGLLGGSYYLKRREEKGK 1460
PF-643 MRSA (C) VRCRL 1461
S. pneumoniae (R)
E. faecalis (R)
PF-644 S. pneumoniae (H) TSGLIIGENGLNGL 1462
PF-645 C. albicans (B) SNSVQQG 1463
S. pneumoniae (I)
PF-646 C. albicans (B) APASPGRRPG 1464
S. pneumoniae (H)
PF-647 C. albicans (B) GTFLGQKCAAATAS 1465
S. pneumoniae (R)
PF-649 E. faecalis (R) CPRYPFVDVGPAGPWRARWRVGS 1466
PF-651 S. pneumoniae (H) PRWPTGAGRHR 1467
PF-652 S. pneumoniae (A) FLAPARPDLQAQRQALAQ 1468
PF-653 S. pneumoniae (H) QSVHPLPAETPVADVI 1469
PF-654 C. albicans (B) LSGRLAGRR 1470
MRSA (R)
S. pneumoniae (A)
PF-655 S. epidermidis (R) DAPCFDDQFGDLKCQMC 1471
B. subtilis (H)
MRSA (M)
S. pneumoniae (H)
PF-656 MRSA (R) RGMFVPFHDVDCVQ 1472
PF-657 S. epidermidis (C) YVANYTITQFGRDFDDRLAVAIHFA 1473
MRSA (D)
S. pneumoniae (H)
E. faecalis (D)
C. jeikeium (D)
PF-658 MRSA (R) PTTPPPTTPPEIPTGGTVIST 1474
S. pneumoniae (H)
PF-659 S. epidermidis (M) TVIST 1475
B. subtilis (H)
MRSA (R)
S. pneumoniae (C)
PF-660 S. pneumoniae (H) TDPQATAAPRRRTSPR 1476
PF-661 MRSA (R) PDEDIRRRAILPPAGPCRPMSPE 1477
PF-662 S. pneumoniae (A) GKQSRAHGPVASRREFRRKSG 1478
PF-663 S. pneumoniae (A) ATLIPRKA 1479
PF-664 S. epidermidis (M) DQLCVEYPARVSTG 1480
MRSA (R)
S. pneumoniae (M)
E. faecalis (R)
PF-665 S. pneumoniae (H) VLRVATAVGEVPTGL 1481
PF-666 S. pneumoniae (A) PNRRSRPR 1482
PF-667 S. epidermidis (R) PAHQRLRIDQRLVADRDMVQDYES 1483
MRSA (R)
S. pneumoniae (R)
E. faecalis (R)
PF-668 S. epidermidis (M) TNAESMALAFRGRVHMSVNIAGLT 1484
B. subtilis (A)
C. albicans (A)
MRSA (R)
S. pneumoniae (M)
E. faecalis (D)
C. jeikeium (D)
PF-670 B. subtilis (H) TVIVAPMHSGV 1485
S. pneumoniae (H)
PF-672 S. epidermidis (I) MRFGSLALVAYDSAIKHSWPRPSSVRR 1486
B. subtilis (I) LRM
C. albicans (I)
MRSA (I)
S. pneumoniae (I)
E. faecalis (I)
C. jeikeium (R)
PF-675 S. pneumoniae (C) EIIPISPTRRCEMHTMSSAEYRGL 1487
E. faecalis (R)
PF-677 S. epidermidis (R) TCRGAGMH 1488
MRSA (D)
S. pneumoniae (D)
E. faecalis (R)
PF-680 MRSA (R) ADPHPTTGI 1489
PF-681 S. epidermidis (M) TALTTVGVSGARLITYCVGVEDI 1490
MRSA (M)
S. pneumoniae (M)
E. faecalis (R)
C. jeikeium (R)
PF-682 S. pneumoniae (A) RRGKSEQGLSRR 1491
PF-683 S. epidermidis (R) LWPVA 1492
MRSA (R)
S. pneumoniae (H)
PF-684 C. albicans (B) RKLSLASGFALWRRSLV 1493
S. pneumoniae (C)
E. faecalis (A)
PF-685 S. epidermidis (M) PTLWLACL 1494
MRSA (M)
S. pneumoniae (M)
E. faecalis (R)
C. jeikeium (R)
PF-686 S. epidermidis (H) LAVLMGYIGYRGWSGKRHINRQ 1495
B. subtilis (I)
C. albicans (B)
MRSA (M)
S. pneumoniae (A)
E. faecalis (R)
PF-687 S. pneumoniae (A) AKRVLSLAVAPHRRQPVQGT 1496
PF-688 S. pneumoniae (A) ARNHAVIPAG 1497
PF-690 S. epidermidis (R) MIPLAGDPVSSHRTVEFGVLGTYLVSG 1498
MRSA (R) GSL
S. pneumoniae (M)
E. faecalis (R)
PF-691 S. pneumoniae (R) HRTVEFGVLGTYLVSGGSL 1499
PF-692 MRSA (R) GVAREDPLEPDPLAPIIDDSR 1500
PF-693 S. pneumoniae (A) PDPAR 1501
PF-694 MRSA (R) DLIRPLYSMSAPSVA 1502
S. pneumoniae (A)
PF-695 MRSA (R) ALSVMLGNIPLVVPNANQL 1503
S. pneumoniae (C)
E. faecalis (R)
PF-696 S. pneumoniae (H) IRSGISAAYARPLR 1504
PF-697 C. albicans (H) RADARAK 1505
S. pneumoniae (H)
PF-698 C. albicans (H) SSGRAGVKCRRPTGR 1506
S. pneumoniae (A)
E. faecalis (A)
PF-699 S. pneumoniae (A) GRAGVKCRRPTGR 1507
PF-700 S. pneumoniae (C) LNWPFTGR 1508
PF-702 S. pneumoniae (H) LSGRLAGRR 1509
PF-704 S. pneumoniae (C) APAARAAL 1510
PF-737 S. pneumoniae (D) KSSGSSASASSTAGGSSSK 1511
PF-738 MRSA (M) KSGATSAASGAKSGASS 1512
PF-741 S. mutans (D) AKREDTVAAQIGANILNLIQ 1513
S. epidermidis (C)
M. luteus (C)
P. mirabilis (C)
E. coli (C)
MRSA (C)
S. pneumoniae (D)
PF-744 S. pneumoniae (H) LGVGTFVGKVLIKNQQKQKSKKKAQ 1514
PF-745 S. mutans (D) ANSQNSLFSNRSSFKSIFDKKSNITTNA 1515
M. luteus (C) TTPNSNIIIN
MRSA (C)
S. pneumoniae (C)
PF-746 S. mutans (D) FLGNSQYFTRK 1516
S. epidermidis (C)
M. luteus (C)
E. coli (C)
P. aeruginosa (A)
MRSA (C)
S. pneumoniae (C)
PF-748 S. pneumoniae (H) FQGFFDVAVNKWWEEHNKAKLWKN 1517
VKGKFLEGEGEEEDDE
PF-749 S. pneumoniae (H) GVNKWWEEHNKAKLWKNVKGKFLE 1518
GEGEEEDDE
PF-752 S. pneumoniae (C) LHVIRPRPELSELKFPITKILKVNKQGL 1519
KK
PF-756 S. pneumoniae (A) DALLRLA 1520
PF-757 S. pneumoniae (H) PQAISSVQQNA 1521
PF-760 S. epidermidis (M) DHITLDDYEIHDGFNFELYYG 1522
MRSA (M)
S. pneumoniae (C)
PF-761 S. mutans (D) SKFELVNYASGCSCGADCKCASETECK 1523
S. epidermidis (C) CASKK
M. luteus (C)
E. coli (C)
P. aeruginosa (C)
MRSA (D)
S. pneumoniae (C)
PF-762 S. pneumoniae (H) PAPAPSAPAPAPEQPEQPA 1524
PF-763 S. epidermidis (M) GIWMARNYFHRSSIRKVYVESDKEYE 1525
M. luteus (C) RVHPMQKIQYEGNYKSQ
MRSA (D)
S. pneumoniae (C)
PF-764 MRSA (D) GYFEPGKRD 1526
S. pneumoniae (H)
PF-770 S. mutans (D) GVGIGFIMMGVVGYAVKLVHIPIRYLIV 1527
S. epidermidis (D)
M. luteus (C)
P. mirabilis (C)
E. coli (C)
MRSA (D)
S. pneumoniae (C)
PF-776 S. mutans (D) VSILLYLSATIILPNVLRLLVARAIIVRV 1528
S. epidermidis (D)
M. luteus (C)
E. coli (C)
MRSA (D)
S. pneumoniae (C)
PF-C052 P. gingivalis (H) SRFRNGV 1529
PF-C055 F. nucleatum (T) YNLSIYIYFLHTITIAGLITLPFII 1530
S. mutans (I)
PF-C057 S. mutans (I) YFWWYWVQDCIPYKNNEVWLELSNN 1531
MK
PF-C058 S. mutans (F) FETGFGDGYYMSLWGLNEKDEVCKV 1532
VIPFINPELID
PF-C061 F. nucleatum (T) TLNYKKMFFSVIFLLGLNYLICNSPLFF 1533
S. mutans (F) KQIEF
PF-C062 F. nucleatum (T) PLARATEVVATLFIICSLLLYLTR 1534
S. mutans (I)
PF-C064 F. nucleatum (T) DEEALEMGANLYAQFAIDFLNSKK 1535
PF-C065 F. nucleatum (T) DEERYSDSYFLKEKVFYLILALFLILFH 1536
QKYLYFLEIITI
PF-C069 F. nucleatum (T) NALMLREMQLAKNIKVEVTDVLSNKK 1537
YC
PF-C071 F. nucleatum (T) QVIVKIL 1538
PF-C072 F. nucleatum (T) KKMFSLIRKVNWIFFILFIVLDLTNVFP 1539
P. gingivalis (T) LIRTILFAILSRQ
S. mutans (F)
PF-C075 F. nucleatum (T) KALVISVFAIVFSIIFVKFFYWRDKK 1540
P. gingivalis (R)
S. mutans (F)
PF-C084 F. nucleatum (T) FFSVIFLFGLNYLICNSPLFNILR 1541
P. gingivalis (R)
S. mutans (F)
PF-C085 S. mutans (F) KKFKIFVIINWFYHKYIILNFEENF 1542
PF-C086 F. nucleatum (T) ELFFTILSDCNELFLLHLLQQPLFYIKK 1543
GK
PF-C088 F. nucleatum (H) DIANNILNSVSERLIIA 1544
P. gingivalis (R)
S. mutans (I)
PF-C089 P. gingivalis (R) MPKRHYYKLEAKALQFGLPFAYSPIQL 1545
LK
PF-C091 F. nucleatum (T) ASNTPRFVRLTLFNFYSKIWNVTHLFLF 1546
NNL
PF-C095 F. nucleatum (T) LLALNMNEDTYYFELFFIFDNQNKKW 1547
LIFDLKERG
PF-C098 F. nucleatum (T) PETKGKVSAFVFGIVVANVIAVVYILY 1548
S. mutans (F) MLREIGIIQ
PF-C120 F. nucleatum (T) ASLSTMTFKVMELKELIILLCGLTMLMI 1549
QTEFV
PF-C131 F. nucleatum (T) QWIVAKREIRMHIYCHISVIHVIIFFG 1550
S. mutans (F)
PF-C135 F. nucleatum (C) KNTHAYLRVLRLSSLILSYQASVYPLF 1551
S. mutans (F) AYLCQQKDY
PF-C136 F. nucleatum (C) LILSYQASVYPLFAYLCQQKDY 1552
P. gingivalis (R)
PF-C137 F. nucleatum (T) QRMYWFKRGFETGDFSAGDTFAELK 1553
PF-C139 S. mutans (F) LLASHPERLSLGVFFVYRVLHLLLENT 1554
PF-C142 S. mutans (I) DFPPLSFFRRRFHAYTAPIDNFFGANPF 1555
PF-C143 F. nucleatum (C) VVFGGGDRLV 1556
PF-C145 F. nucleatum (C) YGKESDP 1557
S. mutans (I)
PF-C180 P. gingivalis (R) TVEELDKAFTWGAAAALAIGVIAINVG 1558
S. mutans (S) LAAGYCYNNNDVF
PF-C181 F. nucleatum (T) KMRAGQVVFIYKLILVLLFYVLQKLFD 1559
LKKGCF
PF-C194 F. nucleatum (T) NTNDLLQAFELMGLGMAGVFIVLGILY 1560
P. gingivalis (T) IVAELLIKIFPVNN
S. mutans (F)
PF-C214 F. nucleatum (T) GGHKQLVIEPLVSQ 1561
PF-C281 S. mutans (F) KKEKLLTAIRLQHRAEIRGYFTIFFLFFRI 1562
PF-C290 S. mutans (F) GNVHPESDFHNLIQFIKTFLYFTIFFKYFL 1563
PF-C291 F. nucleatum (T) HPFLTGTGCPLFLIFRLFFVKAYFSFTVF 1564
S. mutans (F)
PF-C293 F. nucleatum (T) IIIILPKIYLVCKTV 1565
P. gingivalis (R)
S. mutans (F)
PF-S003 S. epidermidis (R) ALALLKQDLLNFEGRGRIITSTYLQFNE 1566
M. luteus (R) GCVP
B. subtilis (A)
P. aeruginosa (A)
C. albicans (A)
MRSA (M)
S. pneumoniae (D)
C. jeikeium (D)
C. jejuni (D)
Key to Abbreviations:
(A) Peptide aggregates;
(B) Less hyphal formation;
(C) Clumps;
(D) Diffuse clumps and small polyps;
(F) Diffuse growth;
(H) Thin;
(I) Growth inhibition;
(M) Microcolony formation;
(R) Rippled;
(S) Small polyps;
(T) Thick;
(W) Halo formation on top, microlonies on bottom.
These data thus indicate peptide-mediated interruption of bacterial biofilm formation processes, cellular metabolism, cellular import/export, nutrient acquisition, quorum sensing and communication, motility, chemotaxis, replication, translation, and/or transcription. Accordingly, without being bound to a particular theory, it is believed that the alteration of one or more of these basic pathways is important to pathogenesis, or the stopping thereof.
In certain embodiments, the amino acid sequence of the antimicrobial peptides comprises or consists of a single amino acid sequence, e.g., as listed above in Tables 4 and/or 5, and/or Table 15, and/or below in Table 14. In certain embodiments the amino acid sequence of the antimicrobial peptides comprises two copies, three copies, four copies, five copies six copies or more of one or more of the amino acid sequences listed in Tables 4, and/or 5, and/or Table 15, and/or Table 14. Thus, compound antimicrobial constructs are contemplated where the construct comprises multiple domains each having antimicrobial activity. The AMP domains comprising such a construct can be the same or different. In certain embodiments the construct comprises at least 2, at least 3, at least 4, at least 5, at least 6, at least 7, or at least 8 different AMP domains each domain comprising a different AMP sequence.
Various AMP domains comprising such a construct can be joined directly to each other or two or more of such domains can be attached to each other via a linker. An illustrative, but non-limiting, list of suitable linkers is provided in Table 16. Thus, in certain embodiments, two or more AMP domains comprising a compound AMP construct are chemically conjugated together.
In certain embodiments the two or more AMP domains comprising the AMP construct are joined by a peptide linker. Where all the AMP domains are attached directly to each other or are joined by peptide linkers, the entire construct can be provided as a single-chain peptide (fusion protein).
In various embodiments, the antimicrobial peptides described herein comprise one or more of the amino acid sequences shown in Tables 4, and/or 5, and/or 15 and/or 14 (and/or the retro, inverso, retroinverso, etc. forms of such sequences). In certain embodiments the peptides range in length up to about 100 amino acids in length, preferably up to about 80, about 70, about 60, or about 51 amino acids in length. In certain embodiments the peptides range in length from about 8 amino acids up to about 100 amino acids 80 amino acids, 60 amino acids or about 51 amino acids in length. In certain embodiments the peptides range in length from about 8 up to about 50, 40, 30, 20, 15, 15, 13, or 12 amino acids in length.
As shown in Tables 4, and/or 5, and/or 15 and/or 14, the various amino acid sequences described herein are effective against particular microorganisms. The range of activity of the peptides or compositions comprising such peptides can be increased by including amino acid sequences effective against different microorganisms either as separate components and/or as multiple domains within a single construct.
TABLE 6
Illustrative target microorganisms and peptides effective against that target.
Gram Positive Bacteria:
A. naeslundii PF-531, PF-527, PF-672, PF-545, PF-168, PF-448, PF-525, PF-529, PF-
148
B. subtilis PF-002, PF-005, PF-006, PF-040, PF-053, PF-056, PF-061, PF-063, PF-
067, PF-068, PF-069, PF-070, PF-071, PF-145, PF-148, PF-171, PF-175,
PF-283, PF-289, PF-292, PF-296, PF-297, PF-301, PF-303, PF-305, PF-
306, PF-307, PF-318, PF-319, PF-322, PF-335, PF-339, PF-342, PF-497,
PF-499, PF-527, PF-531, PF-545, PF-547, PF-548, PF-549, PF-550, PF-
552, PF-553, PF-554, PF-556, PF-557, PF-558, PF-559, PF-560, PF-561,
PF-563, PF-564, PF-565, PF-566, PF-569, PF-571, PF-572, PF-574, PF-
632, PF-636, PF-655, PF-659, PF-668, PF-670, PF-672, PF-686, PF-998,
PF-2003
C. difficile PF-522, PF-531, PF-538
C. jeikeium PF-001, PF-003, PF-004, PF-101, PF-011, PF-012, PF-013, PF-021, PF-
022, PF-025, PF-028, PF-030, PF-032, PF-033, PF-036, PF-037, PF-040,
PF-042, PF-043, PF-046, PF-048, PF-052, PF-053, PF-056, PF-057, PF-
063, PF-065, PF-067, PF-068, PF-073, PF-075, PF-076, PF-099, PF-124,
PF-127, PF-129, PF-133, PF-135, PF-137, PF-139, PF-140, PF-145, PF-
148, PF-164, PF-173, PF-176, PF-186, PF-188, PF-190, PF-191, PF-196,
PF-199, PF-203, PF-204, PF-208, PF-527, PF-531, PF-545, PF-546, PF-
548, PF-553, PF-556, PF-564, PF-566, PF-567, PF-575, PF-622, PF-523,
PF-629, PF-632, PF-635, PF-637, PF-657, PF-668, PF-672, PF-681, PF-
685, PF-S003
E. faecalis PF-007, PF-053, PF-057, PF-068, PF-347, PF-349, PF-355, PF-356, PF-
363, PF-366, PF-369, PF-374, PF-375, PF-376, PF-379, PF-380, PF-381,
PF-386, PF-387, PF-389, PF-390, PF-392, PF-393, PF-394, PF-396, PF-
398, PF-399, PF-401, PF-407, PF-410, PF-411, PF-418, PF-422, PF-425,
PF-426, PF-427, PF-429, PF-431, PF-432, PF-439, PF-440, PF-444, PF-
447, PF-450, PF-451, PF-452, PF-454, PF-456, PF-460, PF-461, PF-469,
PF-470, PF-471, PF-472, PF-473, PF-474, PF-475, PF-480, PF-484, PF-
514, PF-518, PF-519, PF-524, PF-530, PF-532, PF-533, PF-534, PF-536,
PF-544, PF-545, PF-546, PF-547, PF-556, PF-577, PF-581, PF-582, PF-
584, PF-585, PF-586, PF-588, PF-591, PF-592, PF-593, PF-594, PF-595,
PF-596, PF-597, PF-598, PF-599, PF-601, PF-602, PF-604, PF-605, PF-
607, PF-609, PF-610, PF-613, PF-614, PF-615, PF-616, PF-617, PF-618,
PF-621, PF-622, PF-623, PF-627, PF-629, PF-631, PF-632, PF-635, PF-
636, PF-637, PF-638, PF-639, PF-640, PF-643, PF-649, PF-657, PF-664,
PF-667, PF-668, PF-672, PF-675, PF-677, PF-681, PF-684, PF-685, PF-
686, PF-690, PF-695, PF-698
M. luteus PF-001, PF-003, PF-004, PF-006, PF-007, PF-010, PF-012, PF-013, PF-
020, PF-021, PF-022, PF-025, PF-030, PF-036, PF-037, PF-040, PF-042,
PF-043, PF-051, PF-052, PF-053, PF-056, PF-057, PF-063, PF-067, PF-
068, PF-071, PF-073, PF-075, PF-076, PF-125, PF-127, PF-137, PF-139,
PF-140, PF-145, PF-148, PF-171, PF-175, PF-176, PF-199, PF-204, PF-
212, PF-215, PF-224, PF-226, PF-234, PF-235, PF-249, PF-250, PF-255,
PF-257, PF-264, PF-270, PF-271, PF-274, PF-276, PF-278, PF-357, PF-
527, PF-543, PF-548, PF-556, PF-562, PF-566, PF-567, PF-578, PF-580,
PF-600, PF-603, PF-612, PF-624, PF-634, PF-741, PF-745, PF-746, PF-
761, PF-763, PF-770, PF-776, PF-S003
MRSA PF-001, PF-003, PF-004, PF-006, PF-007, PF-010, PF-011, PF-012, PF-
013, PF-015, PF-017, PF-019, PF-020, PF-021, PF-022, PF-023, PF-024,
PF-025, PF-026, PF-027, PF-028, PF-029, PF-030, PF-031, PF-033, PF-
035, PF-036, PF-037, PF-040, PF-041, PF-042, PF-043, PF-045, PF-046,
PF-048, PF-049, PF-051, PF-052, PF-053, PF-056, PF-057, PF-058, PF-
063, PF-064, PF-065, PF-066, PF-067, PF-068, PF-071, PF-073, PF-074,
PF-075, PF-076, PF-140, PF-145, PF-148, PF-149, PF-156, PF-168, PF-
171, PF-178, PF-191, PF-209, PF-347, PF-349, PF-350, PF-354, PF-355,
PF-356, PF-357, PF-360, PF-362, PF-366, PF-369, PF-370, PF-373, PF-
374, PF-375, PF-376, PF-378, PF-379, PF-380, PF-381, PF-382, PF-386,
PF-387, PF-389, PF-390, PF-392, PF-393, PF-394, PF-395, PF-396, PF-
398, PF-399, PF-401, PF-403, PF-404, PF-405, PF-406, PF-407, PF-408,
PF-410, PF-411, PF-413, PF-417, PF-418, PF-422, PF-425, PF-426, PF-
427, PF-429, PF-430, PF-431, PF-432, PF-439, PF-440, PF-442, PF-443,
PF-444, PF-447, PF-450, PF-451, PF-452, PF-453, PF-454, PF-458, PF-
460, PF-461, PF-469, PF-471, PF-472, PF-473, PF-474, PF-475, PF-478,
PF-480, PF-518, PF-519, PF-524, PF-526, PF-527, PF-528, PF-530, PF-
532, PF-533, PF-534, PF-536, PF-539, PF-540, PF-543, PF-544, PF-545,
PF-546, PF-547, PF-548, PF-549, PF-551, PF-553, PF-555, PF-556, PF-
558, PF-560, PF-561, PF-562, PF-564, PF-565, PF-566, PF-567, PF-576,
PF-577, PF-578, PF-580, PF-581, PF-583, PF-584, PF-585, PF-586, PF-
589, PF-592, PF-595, PF-596, PF-598, PF-599, PF-600, PF-603, PF-605,
PF-606, PF-607, PF-609, PF-610, PF-612, PF-613, PF-615, PF-619, PF-
622, PF-623, PF-624, PF-627, PF-629, PF-630, PF-632, PF-634, PF-635,
PF-637, PF-638, PF-639, PF-652, PF-643, PF-654, PF-655, PF-656, PF-
657, PF-658, PF-659, PF-661, PF-664, PF-667, PF-778, PF-672, PF-677,
PF-680, PF-683, PF-685, PF-686, PF-690, PF-692, PF-694, PF-695, PF-
738, PF-741, PF-745, PF-746, PF-760, PF-761, PF-763, PF-764, PF-770,
PF-776, PF-S003
S. epidermidis PF-001, PF-003, PF-004, PF-006, PF-007, PF-009, PF-010, PF-012, PF-
013, PF-020, PF-021, PF-022, PF-024, PF-025, PF-027, PF-028, PF-030,
PF-032, PF-033, PF-034, PF-036, PF-037, PF-040, PF-041, PF-042, PF-
043, PF-046, PF-048, PF-051, PF-052, PF-953, PF-956, PF-957, PF-961,
PF-963, PF-964, PF-965, PF-967, PF-968, PF-971, PF-073, PF-074, PF-
075, PF-076, PF-099, PF-123, PF-124, PF-125, PF-127, PF-128, PF-129,
PF-137, PF-139, PF-140, PF-145, PF-148, PF-153, PF-157, PF-171, PF-
173, PF-176, PF-178, PF-180, PF-186, PF-190, PF-191, PF-192, PF-196,
PF-199, PF-203, PF-204, PF-208, PF-209, PF-226, PF-233, PF-273, PF-
278, PF-283, PF-290, PF-292, PF-293, PF-294, PF-296, PF-297, PF-301,
PF-307, PF-310, PF-313, PF-318, PF-319, PF-322, PF-335, PF-339, PF-
342, PF-347, PF-349, PF-350, PF-355, PF-356, PF-357, PF-360, PF-363,
PF-366, PF-369, PF-370, PF-373, PF-374, PF-375, PF-376, PF-378, PF-
379, PF-380, PF-381, PF-383, PF-386, PF-387, PF-389, PF-390, PF-393,
PF-395, PF-396, PF-397, PF-398, PF-399, PF-401, PF-403, PF-404, PF-
406, PF-407, PF-408, PF-410, PF-411, PF-413, PF-417, PF-418, PF-422,
PF-425, PF-246, PF-249, PF-430, PF-431, PF-432, PF-439, PF-440, PF-
444, PF-447, PF-451, PF-452, PF-453, PF-454, PF-460, PF-469, PF-471,
PF-473, PF-474, PF-475, PF-478, PF-480, PF-514, PF-518, PF-526, PF-
527, PF-528, PF-530, PF-531, PF-533, PF-534, PF-536, PF-540, PF-543,
PF-544, PF-546, PF-547, PF-548, PF-556, PF-558, PF-562, PF-576, PF-
577, PF-578, PF-580, PF-583, PF-584, PF-585, PF-586, PF-592, PF-595,
PF-596, PF-598, PF-599, PF-600, PF-603, PF-605, PF-606, PF-607, PF-
610, PF-612, PF-613, PF-614, PF-615, PF-616, PF-619, PF-622, PF-623,
PF-624, PF-627, PF-632, PF-634, PF-635, PF-637, PF-638, PF-655, PF-
657, PF-659, PF-664, PF-667, PF-778, PF-672, PF-677, PF-681, PF-683,
PF-685, PF-686, PF-690, PF-741, PF-746, PF-760, PF-761, PF-763, PF-
770, PF-776, PF-S003
S. mutans G-1, G-2, G-4, G-8, PF-020, PF-040, PF-051, PF-531, PF-543, PF-547,
PF-578, PF-583, PF-600, PF-606, PF-612, PF-624, PF-634, PF-741, PF-
745, PF-746, PF-761, PF-770, PF-776, PF-C055, PF-C057, PF-C058, PF-
C061, PF-C062, PF-C072, PF-C075, PF-C084, PF-C085, PF-C088, PF-
C098, PF-C131, PF-C135, PF-C139, PF-C142, PF-C146, PF-C180, PF-
C194, PF-C281, PF-C290, PF-C291, PF-C293
S. pneumoniae PF-002, PF-005, PF-006, PF-020, PF-033, PF-040, PF-051, PF-053, PF-
056, PF-057, PF-061, PF-063, PF-068, PF-071, PF-073, PF-140, PF-144,
PF-145, PF-148, PF-171, PF-175, PF-178, PF-220, PF-355, PF-356, PF-
357, PF-363, PF-366, PF-380, PF-389, PF-390, PF-393, PF-407, PF-411,
PF-414, PF-415, PF-416, PF-417, PF-418, PF-419, PF-421, PF-422, PF-
423, PF-424, PF-425, PF-426, PF-427, PF-428, PF-429, PF-430, PF-431,
PF-432, PF-433, PF-434, PF-437, PF-439, PF-440, PF-442, PF-443, PF-
444, PF-445, PF-446, PF-447, PF-448, PF-449, PF-450, PF-451, PF-452,
PF-453, PF-454, PF-455, PF-457, PF-458, PF-469, PF-460, PF-461, PF-
462, PF-464, PF-465, PF-466, PF-467, PF-468, PF-469, PF-471, PF-472,
PF-473, PF-474, PF-475, PF-476, PF-477, PF-478, PF-479, PF-480, PF-
482, PF-485, PF-511, PF-512, PF-513, PF-514, PF-515, PF-516, PF-517,
PF-518, PF-519, PF-520, PF-521, PF-522, PF-523, PF-524, PF-525, PF-
526, PF-527, PF-528, PF-529, PF-530, PF-531, PF-532, PF-533, PF-534,
PF-535, PF-536, PF-537, PF-538, PF-539, PF-540, PF-541, PF-542, PF-
543, PF-544, PF-546, PF-548, PF-553, PF-555, PF-556, PF-558, PF-560,
PF-562, PF-563, PF-566, PF-567, PF-572, PF-573, PF-575, PF-576, PF-
577, PF-578, PF-580, PF-581, PF-583, PF-585, PF-585, PF-586, PF-587,
PF-589, PF-591, PF-592, PF-595, PF-596, PF-598, PF-599, PF-600, PF-
603, PF-605, PF-606, PF-607, PF-609, PF-610, PF-612, PF-614, PF-615,
PF-617, PF-618, PF-619, PF-621, PF-622, PF-623, PF-624, PF-625, PF-
626, PF-627, PF-629, PF-631, PF-632, PF-634, PF-635, PF-636, PF-637,
PF-638, PF-639, PF-640, PF-643, PF-644, PF-645, PF-646, PF-647, PF-
651, PF-652, PF-653, PF-654, PF-655, PF-657, PF-658, PF-659, PF-660,
PF-662, PF-663, PF-664, PF-665, PF-666, PF-667, PF-668, PF-670, PF-
672, PF-675, PF-677, PF-681, PF-682, PF-683, PF-684, PF-685, PF-686,
PF-687, PF-688, PF-690, PF-691, PF-693, PF-694, PF-695, PF-696, PF-
697, PF-698, PF-699, PF-700, PF-702, PF-704, PF-737, PF-741, PF-744,
PF-745, PF-746, PF-748, PF-749, PF-752, PF-756, PF-757, PF-760, PF-
761, PF-762, PF-763, PF-764, PF-770, PF-776, PF-S003
Gram Negative Bacteria:
A. baumannii PF-531, PF-006, PF-538, PF-530
C. jejuni PF-006, PF-008, PF-033, PF-040, PF-053, PF-056, PF-057, PF-059, PF-
061, PF-063, PF-067, PF-068, PF-069, PF-071, PF-073, PF-140, PF-145,
PF-148, PF-171, PF-175, PF-355, PF-356, PF-363, PF-366, PF-380, PF-
389, PF-390, PF-392, PF-393, PF-411, PF-418, PF-422, PF-425, PF-426,
PF-431, PF-432, PF-456, PF-469, PF-470, PF-471, PF-472, PF-473, PF-
474, PF-475, PF-527, PF-548, PF-555, PF-556, PF-558, PF-559, PF-560,
PF-562, PF-563, PF-564, PF-566, PF-567, PF-575, PF-576, PF-577, PF-
581, PF-584, PF-585, PF-586, PF-590, PF-591, PF-592, PF-595, PF-596,
PF-598, PF-599, PF-601, PF-605, PF-607, PF-609, PF-610, PF-614, PF-
615, PF-S003
E. coli PF-007, PF-040, PF-053, PF-057, PF-068, PF-178, PF-344, PF-347, PF-
349, PF-350, PF-355, PF-360, PF-362, PF-363, PF-366, PF-369, PF-370,
PF-374, PF-375, PF-376, PF-379, PF-380, PF-381, PF-383, PF-385, PF-
386, PF-387, PF-390, PF-395, PF-396, PF-398, PF-399, PF-401, PF-403,
PF-410, PF-411, PF-413, PF-418, PF-425, PF-426, PF-427, PF-432, PF-
439, PF-440, PF-443, PF-444, PF-451, PF-452, PF-453, PF-454, PF-460,
PF-469, PF-471, PF-473, PF-474, PF-478, PF-480, PF-514, PF-518, PF-
519, PF-524, PF-526, PF-528, PF-530, PF-531, PF-532, PF-533, PF-534,
PF-536, PF-540, PF-541, PF-543, PF-546, PF-576, PF-577, PF-578, PF-
584, PF-586, PF-592, PF-595, PF-596, PF-598, PF-600, PF-603, PF-605,
PF-606, PF-610, PF-612, PF-615, PF-619, PF-624, PF-634, PF-741, PF-
746, PF-761, PF-770, PF-776
F. nucleatum PF-C055, PF-C061, PF-C062, PF-C064, PF-C065, PF-C069, PF-C071,
PF-C072, PF-C075, PF-C084, PF-C086, PF-C088, PF-C091, PF-C095,
PF-C098, PF-C120, PF-C131, PF-C135, PF-C136, PF-C137, PF-C143,
PF-C145, PF-C181, PF-C194, PF-C214, PF-C291, PF-C293
M. xanthus G-5, G-6, G-7
P. aeruginosa PF-053, PF-063, PF-067, PF-128, PF-140, PF-143, PF-168, PF-204, PF-
209, PF-355, PF-356, PF-366, PF-380, PF-411, PF-425, PF-432, PF-454,
PF-458, PF-471, PF-474, PF-527, PF-531, PF-535, PF-536, PF-575, PF-
577, PF-605, PF-746, PF-761, PF-S003
P. gingivalis PF-C052, PF-C072, PF-C075, PF-C084, PF-C088, PF-C089, PF-C136,
PF-C180, PF-C194, C293
P. mirabilis PF-040, PF-578, PF-612, PF-624, PF-634, PF-741, PF-770
Yeast Fungi:
A. niger PF-531, PF-527, PF-672, PF-545, PF-168, PF-448, PF-525, PF-529, PF-
148
C. albicans PF-053, PF-056, PF-057, PF-071, PF-140, PF-148, PF-175, PF-278, PF-
307, PF-425, PF-426, PF-474, PF-475, PF-526, PF-527, PF-528, PF-545,
PF-605, PF-606, PF-617, PF-627, PF-632, PF-635, PF-636, PF-639, PF-
640, PF-645, PF-646, PF-647, PF-654, PF-668, PF-672, PF-684, PF-686,
PF-697, PF-698, PF-S003
T. rubrum PF-283, PF-307, PF-527, PF-531, PF-547, PF-672
In certain embodiments the activity against a particular microorganism or group of microorganisms can be increased by increasing the number of peptides or peptide domains with activity against that microorganism or group of microorganisms.
Thus, for example, in certain embodiments, a peptide or composition effective to kill or inhibit the growth and/or proliferation of a yeast or fungus can comprise or more peptides and/or one or more peptide domains having sequences selected from the sequences shown in Tables 4, 5, or 6 (e.g., PF-S003, PF-053, PF-056, PF-057, PF-071, PF-140, PF-148, PF-168, PF-175, PF-278, PF-283, PF-307, PF-425, PF-426, PF-448, PF-474, PF-475, PF-525, PF-526, PF-527, PF-528, PF-529, PF-531, PF-545, PF-547, PF-606, PF-617, PF-627, PF-632, PF-635, PF-636, PF-639, PF-640, PF-645, PF-646, PF-647, PF-654, PF-668, PF-672, PF-684, PF-686, PF-697, and PF-69)8. A peptide or composition effective to kill or inhibit the growth and/or proliferation of Aspergillus niger can comprise one or more peptides and/or one or more peptide domains having sequences selected from the group consisting of PF-531, PF-527, PF-672, PF-545, PF-168, PF-448, PF-525, PF-529, and PF-148. A peptide or composition effective to kill or inhibit the growth and/or proliferation of Candida albicans can comprise one or more peptides and/or one or more peptide domains having sequences selected from the group consisting of PF-053, PF-056, PF-057, PF-071, PF-140, PF-148, PF-175, PF-278, PF-307, PF-425, PF-426, PF-474, PF-475, PF-526, PF-527, PF-528, PF-545, PF-605, PF-606, PF-617, PF-627, PF-632, PF-635, PF-636, PF-639, PF-640, PF-645, PF-646, PF-647, PF-654, PF-668, PF-672, PF-684, PF-686, PF-697, PF-698, and PF-S003. A peptide or composition effective to kill or inhibit the growth and/or proliferation of Trichophyton rubrum can comprise one or more peptides and/or one or more peptide domains having sequences selected from the group consisting of PF-283, PF-307, PF-527, PF-531, PF-547, and PF-672.
In certain embodiments a peptide or composition effective to kill or inhibit the growth and/or proliferation of a bacterium can comprise one or more peptides and/or one or more peptide domains comprising or consisting of sequences identified as having activity against a bacterium in Tables 4, 5, or 6.
In certain embodiments a peptide or composition effective to kill or inhibit the growth and/or proliferation of a gram positive bacterium can comprise one or more peptides and/or one or more peptide domains comprising or consisting of sequences identified as having activity against a gram positive bacterium in Tables 4, 5, or 6. In certain embodiments a peptide or composition effective to kill or inhibit the growth and/or proliferation of a gram negative bacterium can comprise one or more peptides and/or one or more peptide domains comprising or consisting of sequences identified as having activity against a gram negative bacterium in Tables 4, 5, or 6.
In certain embodiments a peptide or composition effective to kill or inhibit the growth and/or proliferation of A. naeslundii can comprise one or more peptides and/or one or more peptide domains comprising or consisting of sequences identified as having activity against A. Naeslundii in Tables 4, 5, or 6 (e.g., from the group consisting of PF-531, PF-527, PF-672, PF-545, PF-168, PF-448, PF-525, PF-529, and PF-148).
In certain embodiments a peptide or composition effective to kill or inhibit the growth and/or proliferation of B. subtilis can comprise one or more peptides and/or one or more peptide domains comprising or consisting of sequences identified as having activity against B. subtilis in Tables 4, 5, or 6 (e.g., from the group consisting of PF-002, PF-005, PF-006, PF-040, PF-053, PF-056, PF-061, PF-063, PF-067, PF-068, PF-069, PF-070, PF-071, PF-145, PF-148, PF-171, PF-175, PF-283, PF-289, PF-292, PF-296, PF-297, PF-301, PF-303, PF-305, PF-306, PF-307, PF-318, PF-319, PF-322, PF-335, PF-339, PF-342, PF-497, PF-499, PF-527, PF-531, PF-545, PF-547, PF-548, PF-549, PF-550, PF-552, PF-553, PF-554, PF-556, PF-557, PF-558, PF-559, PF-560, PF-561, PF-563, PF-564, PF-565, PF-566, PF-569, PF-571, PF-572, PF-574, PF-632, PF-636, PF-655, PF-659, PF-668, PF-670, PF-672, PF-686, PF-998, and PF-2003).
In certain embodiments a peptide or composition effective to kill or inhibit the growth and/or proliferation of C. difficile can comprise one or more peptides and/or one or more peptide domains comprising or consisting of sequences identified as having activity against C. difficile in Tables 4, 5, or 6 (e.g., from the group consisting of PF-522, PF-531, and PF-538).
In certain embodiments a peptide or composition effective to kill or inhibit the growth and/or proliferation of C. jeikeium can comprise one or more peptides and/or one or more peptide domains comprising or consisting of sequences identified as having activity against C. jeikeium in Tables 4, 5, or 6 (e.g., from the group consisting of PF-001, PF-003, PF-004, PF-101, PF-011, PF-012, PF-013, PF-021, PF-022, PF-025, PF-028, PF-030, PF-032, PF-033, PF-036, PF-037, PF-040, PF-042, PF-043, PF-046, PF-048, PF-052, PF-053, PF-056, PF-057, PF-063, PF-065, PF-067, PF-068, PF-073, PF-075, PF-076, PF-099, PF-124, PF-127, PF-129, PF-133, PF-135, PF-137, PF-139, PF-140, PF-145, PF-148, PF-164, PF-173, PF-176, PF-186, PF-188, PF-190, PF-191, PF-196, PF-199, PF-203, PF-204, PF-208, PF-527, PF-531, PF-545, PF-546, PF-548, PF-553, PF-556, PF-564, PF-566, PF-567, PF-575, PF-622, PF-523, PF-629, PF-632, PF-635, PF-637, PF-657, PF-668, PF-672, PF-681, PF-685, and PF-S003).
In certain embodiments a peptide or composition effective to kill or inhibit the growth and/or proliferation of E. faecalis can comprise one or more peptides and/or one or more peptide domains comprising or consisting of sequences identified as having activity against E. faecalis in Tables 4, 5, or 6 (e.g., from the group consisting of PF-007, PF-053, PF-057, PF-068, PF-347, PF-349, PF-355, PF-356, PF-363, PF-366, PF-369, PF-374, PF-375, PF-376, PF-379, PF-380, PF-381, PF-386, PF-387, PF-389, PF-390, PF-392, PF-393, PF-394, PF-396, PF-398, PF-399, PF-401, PF-407, PF-410, PF-411, PF-418, PF-422, PF-425, PF-426, PF-427, PF-429, PF-431, PF-432, PF-439, PF-440, PF-444, PF-447, PF-450, PF-451, PF-452, PF-454, PF-456, PF-460, PF-461, PF-469, PF-470, PF-471, PF-472, PF-473, PF-474, PF-475, PF-480, PF-484, PF-514, PF-518, PF-519, PF-524, PF-530, PF-532, PF-533, PF-534, PF-536, PF-544, PF-545, PF-546, PF-547, PF-556, PF-577, PF-581, PF-582, PF-584, PF-585, PF-586, PF-588, PF-591, PF-592, PF-593, PF-594, PF-595, PF-596, PF-597, PF-598, PF-599, PF-601, PF-602, PF-604, PF-605, PF-607, PF-609, PF-610, PF-613, PF-614, PF-615, PF-616, PF-617, PF-618, PF-621, PF-622, PF-623, PF-627, PF-629, PF-631, PF-632, PF-635, PF-636, PF-637, PF-638, PF-639, PF-640, PF-643, PF-649, PF-657, PF-664, PF-667, PF-668, PF-672, PF-675, PF-677, PF-681, PF-684, PF-685, PF-686, PF-690, PF-695, and PF-698).
In certain embodiments a peptide or composition effective to kill or inhibit the growth and/or proliferation of M. luteus can comprise one or more peptides and/or one or more peptide domains comprising or consisting of sequences identified as having activity against M. luteus in Tables 4, 5, or 6 (e.g., from the group consisting of PF-001, PF-003, PF-004, PF-006, PF-007, PF-010, PF-012, PF-013, PF-020, PF-021, PF-022, PF-025, PF-030, PF-036, PF-037, PF-040, PF-042, PF-043, PF-051, PF-052, PF-053, PF-056, PF-057, PF-063, PF-067, PF-068, PF-071, PF-073, PF-075, PF-076, PF-125, PF-127, PF-137, PF-139, PF-140, PF-145, PF-148, PF-171, PF-175, PF-176, PF-199, PF-204, PF-212, PF-215, PF-224, PF-226, PF-234, PF-235, PF-249, PF-250, PF-255, PF-257, PF-264, PF-270, PF-271, PF-274, PF-276, PF-278, PF-357, PF-527, PF-543, PF-548, PF-556, PF-562, PF-566, PF-567, PF-578, PF-580, PF-600, PF-603, PF-612, PF-624, PF-634, PF-741, PF-745, PF-746, PF-761, PF-763, PF-770, PF-776, and PF-S003).
In certain embodiments a peptide or composition effective to kill or inhibit the growth and/or proliferation of MRSA can comprise one or more peptides and/or one or more peptide domains comprising or consisting of sequences identified as having activity against MRSA in Tables 4, 5, or 6 (e.g., from the group consisting of PF-001, PF-003, PF-004, PF-006, PF-007, PF-010, PF-011, PF-012, PF-013, PF-015, PF-017, PF-019, PF-020, PF-021, PF-022, PF-023, PF-024, PF-025, PF-026, PF-027, PF-028, PF-029, PF-030, PF-031, PF-033, PF-035, PF-036, PF-037, PF-040, PF-041, PF-042, PF-043, PF-045, PF-046, PF-048, PF-049, PF-051, PF-052, PF-053, PF-056, PF-057, PF-058, PF-063, PF-064, PF-065, PF-066, PF-067, PF-068, PF-071, PF-073, PF-074, PF-075, PF-076, PF-140, PF-145, PF-148, PF-149, PF-156, PF-168, PF-171, PF-178, PF-191, PF-209, PF-347, PF-349, PF-350, PF-354, PF-355, PF-356, PF-357, PF-360, PF-362, PF-366, PF-369, PF-370, PF-373, PF-374, PF-375, PF-376, PF-378, PF-379, PF-380, PF-381, PF-382, PF-386, PF-387, PF-389, PF-390, PF-392, PF-393, PF-394, PF-395, PF-396, PF-398, PF-399, PF-401, PF-403, PF-404, PF-405, PF-406, PF-407, PF-408, PF-410, PF-411, PF-413, PF-417, PF-418, PF-422, PF-425, PF-426, PF-427, PF-429, PF-430, PF-431, PF-432, PF-439, PF-440, PF-442, PF-443, PF-444, PF-447, PF-450, PF-451, PF-452, PF-453, PF-454, PF-458, PF-460, PF-461, PF-469, PF-471, PF-472, PF-473, PF-474, PF-475, PF-478, PF-480, PF-518, PF-519, PF-524, PF-526, PF-527, PF-528, PF-530, PF-532, PF-533, PF-534, PF-536, PF-539, PF-540, PF-543, PF-544, PF-545, PF-546, PF-547, PF-548, PF-549, PF-551, PF-553, PF-555, PF-556, PF-558, PF-560, PF-561, PF-562, PF-564, PF-565, PF-566, PF-567, PF-576, PF-577, PF-578, PF-580, PF-581, PF-583, PF-584, PF-585, PF-586, PF-589, PF-592, PF-595, PF-596, PF-598, PF-599, PF-600, PF-603, PF-605, PF-606, PF-607, PF-609, PF-610, PF-612, PF-613, PF-615, PF-619, PF-622, PF-623, PF-624, PF-627, PF-629, PF-630, PF-632, PF-634, PF-635, PF-637, PF-638, PF-639, PF-652, PF-643, PF-654, PF-655, PF-656, PF-657, PF-658, PF-659, PF-661, PF-664, PF-667, PF-778, PF-672, PF-677, PF-680, PF-683, PF-685, PF-686, PF-690, PF-692, PF-694, PF-695, PF-738, PF-741, PF-745, PF-746, PF-760, PF-761, PF-763, PF-764, PF-770, PF-776, and PF-S003).
In certain embodiments a peptide or composition effective to kill or inhibit the growth and/or proliferation of S. epidermidis can comprise one or more peptides and/or one or more peptide domains comprising or consisting of sequences identified as having activity against of S. epidermidis in Tables 4, 5, or 6 (e.g., from the group consisting of PF-001, PF-003, PF-004, PF-006, PF-007, PF-009, PF-010, PF-012, PF-013, PF-020, PF-021, PF-022, PF-024, PF-025, PF-027, PF-028, PF-030, PF-032, PF-033, PF-034, PF-036, PF-037, PF-040, PF-041, PF-042, PF-043, PF-046, PF-048, PF-051, PF-052, PF-953, PF-956, PF-957, PF-961, PF-963, PF-964, PF-965, PF-967, PF-968, PF-971, PF-073, PF-074, PF-075, PF-076, PF-099, PF-123, PF-124, PF-125, PF-127, PF-128, PF-129, PF-137, PF-139, PF-140, PF-145, PF-148, PF-153, PF-157, PF-171, PF-173, PF-176, PF-178, PF-180, PF-186, PF-190, PF-191, PF-192, PF-196, PF-199, PF-203, PF-204, PF-208, PF-209, PF-226, PF-233, PF-273, PF-278, PF-283, PF-290, PF-292, PF-293, PF-294, PF-296, PF-297, PF-301, PF-307, PF-310, PF-313, PF-318, PF-319, PF-322, PF-335, PF-339, PF-342, PF-347, PF-349, PF-350, PF-355, PF-356, PF-357, PF-360, PF-363, PF-366, PF-369, PF-370, PF-373, PF-374, PF-375, PF-376, PF-378, PF-379, PF-380, PF-381, PF-383, PF-386, PF-387, PF-389, PF-390, PF-393, PF-395, PF-396, PF-397, PF-398, PF-399, PF-401, PF-403, PF-404, PF-406, PF-407, PF-408, PF-410, PF-411, PF-413, PF-417, PF-418, PF-422, PF-425, PF-246, PF-249, PF-430, PF-431, PF-432, PF-439, PF-440, PF-444, PF-447, PF-451, PF-452, PF-453, PF-454, PF-460, PF-469, PF-471, PF-473, PF-474, PF-475, PF-478, PF-480, PF-514, PF-518, PF-526, PF-527, PF-528, PF-530, PF-531, PF-533, PF-534, PF-536, PF-540, PF-543, PF-544, PF-546, PF-547, PF-548, PF-556, PF-558, PF-562, PF-576, PF-577, PF-578, PF-580, PF-583, PF-584, PF-585, PF-586, PF-592, PF-595, PF-596, PF-598, PF-599, PF-600, PF-603, PF-605, PF-606, PF-607, PF-610, PF-612, PF-613, PF-614, PF-615, PF-616, PF-619, PF-622, PF-623, PF-624, PF-627, PF-632, PF-634, PF-635, PF-637, PF-638, PF-655, PF-657, PF-659, PF-664, PF-667, PF-778, PF-672, PF-677, PF-681, PF-683, PF-685, PF-686, PF-690, PF-741, PF-746, PF-760, PF-761, PF-763, PF-770, PF-776, and PF-S003).
In certain embodiments a peptide or composition effective to kill or inhibit the growth and/or proliferation of S. mutans can comprise one or more peptides and/or one or more peptide domains comprising or consisting of sequences identified as having activity against S. mutans in Tables 4, 5, or 6 (e.g., from the group consisting of G-1, G-2, G-4, G-8, PF-020, PF-040, PF-051, PF-531, PF-543, PF-547, PF-578, PF-583, PF-600, PF-606, PF-612, PF-624, PF-634, PF-741, PF-745, PF-746, PF-761, PF-770, PF-776, PF-C055, PF-C057, PF-C058, PF-C061, PF-C062, PF-C072, PF-C075, PF-C084, PF-C085, PF-C088, PF-C098, PF-C131, PF-C135, PF-C139, PF-C142, PF-C146, PF-C180, PF-C194, PF-C281, PF-C290, PF-C291, PF-C293
In certain embodiments a peptide or composition effective to kill or inhibit the growth and/or proliferation of S. pneumoniae can comprise one or more peptides and/or one or more peptide domains comprising or consisting of sequences identified as having activity against S. pneumoniae in Tables 4, 5, or 6 (e.g., from the group consisting of PF-002, PF-005, PF-006, PF-020, PF-033, PF-040, PF-051, PF-053, PF-056, PF-057, PF-061, PF-063, PF-068, PF-071, PF-073, PF-140, PF-144, PF-145, PF-148, PF-171, PF-175, PF-178, PF-220, PF-355, PF-356, PF-357, PF-363, PF-366, PF-380, PF-389, PF-390, PF-393, PF-407, PF-411, PF-414, PF-415, PF-416, PF-417, PF-418, PF-419, PF-421, PF-422, PF-423, PF-424, PF-425, PF-426, PF-427, PF-428, PF-429, PF-430, PF-431, PF-432, PF-433, PF-434, PF-437, PF-439, PF-440, PF-442, PF-443, PF-444, PF-445, PF-446, PF-447, PF-448, PF-449, PF-450, PF-451, PF-452, PF-453, PF-454, PF-455, PF-457, PF-458, PF-469, PF-460, PF-461, PF-462, PF-464, PF-465, PF-466, PF-467, PF-468, PF-469, PF-471, PF-472, PF-473, PF-474, PF-475, PF-476, PF-477, PF-478, PF-479, PF-480, PF-482, PF-485, PF-511, PF-512, PF-513, PF-514, PF-515, PF-516, PF-517, PF-518, PF-519, PF-520, PF-521, PF-522, PF-523, PF-524, PF-525, PF-526, PF-527, PF-528, PF-529, PF-530, PF-531, PF-532, PF-533, PF-534, PF-535, PF-536, PF-537, PF-538, PF-539, PF-540, PF-541, PF-542, PF-543, PF-544, PF-546, PF-548, PF-553, PF-555, PF-556, PF-558, PF-560, PF-562, PF-563, PF-566, PF-567, PF-572, PF-573, PF-575, PF-576, PF-577, PF-578, PF-580, PF-581, PF-583, PF-585, PF-585, PF-586, PF-587, PF-589, PF-591, PF-592, PF-595, PF-596, PF-598, PF-599, PF-600, PF-603, PF-605, PF-606, PF-607, PF-609, PF-610, PF-612, PF-614, PF-615, PF-617, PF-618, PF-619, PF-621, PF-622, PF-623, PF-624, PF-625, PF-626, PF-627, PF-629, PF-631, PF-632, PF-634, PF-635, PF-636, PF-637, PF-638, PF-639, PF-640, PF-643, PF-644, PF-645, PF-646, PF-647, PF-651, PF-652, PF-653, PF-654, PF-655, PF-657, PF-658, PF-659, PF-660, PF-662, PF-663, PF-664, PF-665, PF-666, PF-667, PF-668, PF-670, PF-672, PF-675, PF-677, PF-681, PF-682, PF-683, PF-684, PF-685, PF-686, PF-687, PF-688, PF-690, PF-691, PF-693, PF-694, PF-695, PF-696, PF-697, PF-698, PF-699, PF-700, PF-702, PF-704, PF-737, PF-741, PF-744, PF-745, PF-746, PF-748, PF-749, PF-752, PF-756, PF-757, PF-760, PF-761, PF-762, PF-763, PF-764, PF-770, PF-776, and PF-S003).
In certain embodiments a peptide or composition effective to kill or inhibit the growth and/or proliferation of A. baumannii can comprise one or more peptides and/or one or more peptide domains comprising or consisting of sequences identified as having activity against A. baumannii in Tables 4, 5, or 6 (e.g., from the group consisting of PF-531, PF-006, PF-538, and PF-530).
In certain embodiments a peptide or composition effective to kill or inhibit the growth and/or proliferation of C. jejuni can comprise one or more peptides and/or one or more peptide domains comprising or consisting of sequences identified as having activity against C. jejuni in Tables 4, 5, or 6 (e.g., from the group consisting of PF-006, PF-008, PF-033, PF-040, PF-053, PF-056, PF-057, PF-059, PF-061, PF-063, PF-067, PF-068, PF-069, PF-071, PF-073, PF-140, PF-145, PF-148, PF-171, PF-175, PF-355, PF-356, PF-363, PF-366, PF-380, PF-389, PF-390, PF-392, PF-393, PF-411, PF-418, PF-422, PF-425, PF-426, PF-431, PF-432, PF-456, PF-469, PF-470, PF-471, PF-472, PF-473, PF-474, PF-475, PF-527, PF-548, PF-555, PF-556, PF-558, PF-559, PF-560, PF-562, PF-563, PF-564, PF-566, PF-567, PF-575, PF-576, PF-577, PF-581, PF-584, PF-585, PF-586, PF-590, PF-591, PF-592, PF-595, PF-596, PF-598, PF-599, PF-601, PF-605, PF-607, PF-609, PF-610, PF-614, PF-615, and PF-S003).
In certain embodiments a peptide or composition effective to kill or inhibit the growth and/or proliferation of E. coli can comprise one or more peptides and/or one or more peptide domains comprising or consisting of sequences identified as having activity against E. coli in Tables 4, 5, or 6 (e.g., from the group consisting of PF-007, PF-040, PF-053, PF-057, PF-068, PF-178, PF-344, PF-347, PF-349, PF-350, PF-355, PF-360, PF-362, PF-363, PF-366, PF-369, PF-370, PF-374, PF-375, PF-376, PF-379, PF-380, PF-381, PF-383, PF-385, PF-386, PF-387, PF-390, PF-395, PF-396, PF-398, PF-399, PF-401, PF-403, PF-410, PF-411, PF-413, PF-418, PF-425, PF-426, PF-427, PF-432, PF-439, PF-440, PF-443, PF-444, PF-451, PF-452, PF-453, PF-454, PF-460, PF-469, PF-471, PF-473, PF-474, PF-478, PF-480, PF-514, PF-518, PF-519, PF-524, PF-526, PF-528, PF-530, PF-531, PF-532, PF-533, PF-534, PF-536, PF-540, PF-541, PF-543, PF-546, PF-576, PF-577, PF-578, PF-584, PF-586, PF-592, PF-595, PF-596, PF-598, PF-600, PF-603, PF-605, PF-606, PF-610, PF-612, PF-615, PF-619, PF-624, PF-634, PF-741, PF-746, PF-761, PF-770, and PF-776).
In certain embodiments a peptide or composition effective to kill or inhibit the growth and/or proliferation of F. nucleatum can comprise one or more peptides and/or one or more peptide domains comprising or consisting of sequences identified as having activity against F. nucleatum in Tables 4, 5, or 6 (e.g., from the group consisting of PF-C055, PF-C061, PF-C062, PF-C064, PF-C065, PF-C069, PF-C071, PF-C072, PF-C075, PF-C084, PF-C086, PF-C088, PF-C091, PF-C095, PF-C098, PF-C120, PF-C131, PF-C135, PF-C136, PF-C137, PF-C143, PF-C145, PF-C181, PF-C194, PF-C214, PF-C291, and PF-C293).
In certain embodiments a peptide or composition effective to kill or inhibit the growth and/or proliferation of M. Xanthus can comprise one or more peptides and/or one or more peptide domains comprising or consisting of sequences identified as having activity against M. Xanthus in Tables 4, 5, or 6 (e.g., from the group consisting of G-5, G-6, and G-7).
In certain embodiments a peptide or composition effective to kill or inhibit the growth and/or proliferation of P. aeruginosa can comprise one or more peptides and/or one or more peptide domains comprising or consisting of sequences identified as having activity against P. aeruginosa in Tables 4, 5, or 6 (e.g., from the group consisting of PF-053, PF-063, PF-067, PF-128, PF-140, PF-143, PF-168, PF-204, PF-209, PF-355, PF-356, PF-366, PF-380, PF-411, PF-425, PF-432, PF-454, PF-458, PF-471, PF-474, PF-527, PF-531, PF-535, PF-536, PF-575, PF-577, PF-605, PF-746, PF-761, and PF-S003).
In certain embodiments a peptide or composition effective to kill or inhibit the growth and/or proliferation of P. gingivalis can comprise one or more peptides and/or one or more peptide domains comprising or consisting of sequences identified as having activity against P. gingivalis in Tables 4, 5, or 6 (e.g., from the group consisting of PF-C052, PF-C072, PF-C075, PF-C084, PF-C088, PF-C089, PF-C136, PF-C180, PF-C194, and C293).
In certain embodiments a peptide or composition effective to kill or inhibit the growth and/or proliferation of P. mirabilis can comprise one or more peptides and/or one or more peptide domains comprising or consisting of sequences identified as having activity against P. mirabilis in Tables 4, 5, or 6 (e.g., from the group consisting of PF-040, PF-578, PF-612, PF-624, PF-634, PF-741, and PF-770).
It was also a surprising discovery that a number of novel antimicrobial peptides are characterized by the presence of particular amino acid motifs. Such motifs include KIF, FIK, KIH, HIK, and KIV, as illustrated in Table 7.
TABLE 7
Antimicrobial peptides characterized
by particular motifs.
SEQ ID
Motif Omnibus # Sequence NO
KIF PF-278 LSLATFAKIFMTRSNWSLKRFNRL 1567
PF-C059 QKIIDMSKFLFSLILFIMIVVIYIGKSIGGYSAIVSS 1568
IMLELDTVLYNKKIFFIYK
PF-C073 FESLLPQATKKIVNNKGSKINKIF 1569
PF-C085 KKFKIFVIINWFYHKYIILNFEENF 1570
PF-531 YIQFHLNQQPRPKVKKIKIFL 1571
PF-C194 NTNDLLQAFELMGLGMAGVFIVLGILYIVAELLI 1572
KIFPVNN
PF-C201 IFKLFEEHLLYLLDAFYYSKIFRRLKQGLYRRKE 1573
QPYTQDLFRM
PF-442 MQIFYIKTKIFLSFFLFLLIFSQCFYKIEE 1574
PF-C252 NYRLVNAIFSKIFKKKFIKF 1575
FIK PF-251 MAWKFIKLDKVVSQKECNNFLEKEENKKLLKL 1576
LRIQKNMR
PF-261 MDIWKFIKSFNTVNTYLLLSCVLLIILVLYFYVI 1577
NPA
PF-497 LVLRICTDLFTFIKWTIKQRKS 1578
PF-775 DLCGQEFIKFKTCVTNQLAKK 1579
PF-591 DLLKSLLGQDGAKNDEIIEFIKIIMEK 1580
PF-597 DEIKVSDEEIEKFIKENNL 1581
PF-608 LICEVVKPEEDFIKVKLNEDNVTAKISREFIAKKI 1582
DA
IT-133 YFIKDDNEALSKDWEVIGNDLKGTIDKYGKEFK 1583
VR
PF-C252 NYRLVNAIFSKIFKKKFIKF 1584
PF-C278 DMKIIKLYIKILSFLFIKYCNKKLNSVKLKA 1585
PF-C290 GNVHPESDFHNLIQFIKTFLYFTIFFKYFL 1586
PF-006 MGIIAGIIKFIKGLIEKFTGK 1587
PF-013 LIQKGLNQTFIVVIRLNNFIKKS 1588
PF-040 MIHLTKQNTMEALHFIKQFYDMFFILNFNV 1589
KIH PF-252 MKKLVAALAVIVILTGCVYDPVNYDKIHDQEF 1590
QDHLRQNG
PF-575 LNFRAENKILEKIHISLIDTVEGSA 1591
PF-533 KTPNDKIHKTIIIKHIIL 1592
HIK PF-222 HIKETR 1593
PF-319 SIGSMIGMYSFRHKTKHIKFTFGIPFILFLQFLLV 1594
YFYILK
PF-477 HKNKLNIPHIKS 1595
KIV PF-272 MTLTIKIKHRSKIVPLNLISLVYAFFTYNFVANRI 1596
MFLTND
PF-758 PEIIKIVSGLL 1597
PF-336 MLTSRKKRLKKIVEEQNKKDESI 1598
PF-C073 FESLLPQATKKIVNNKGSKINKIF 1599
PF-721 TEQAKKIVDILNNWLE 1600
PF-730 FEDIEQIIKYHLIDGKIVAPLLLDR 1601
PF-095 KRGSKIVIAIAVVLIVLAGVWVW 1602
PF-028 ALDCSEQSVILWYETILDKIVGVIK 1603
VIK PF-257 VWENRKKYLENEIERHNVFLKLGQEVIKGLNA 1604
LASRGR
PF-226 LMFFSENMDKRDTLSGKFRYFAGSKVIKLMNW 1605
LSENGK
PF-580 EILNNNQVIKELTMKYKTQFESNLGGWTARARR 1606
PF-366 ALCSVIKAIELGIINVHLQ 1607
PF-C092 NGDKKAKEELDKWDEVIKELNIQF 1608
PF-S028 GSVIKKRRKRMSKKKHRKMLRRTRVQRRKLGK 1609
PF-103 VIKISVPGQVQMLIP 1610
PF-527 GSVIKKRRKRMAKKKHRKLLKKTRIQRRRAGK 1611
PF-167 AIEGVIKKGACFKLLRHEMF 1612
PF-C166 KRKHENVIVAEEMRVIKN 1613
PF-007 MGIIAGIIKVIKSLIEQFTGK 1614
PF-071 HCVIGNVVDIANLLKRRAVYRDIADVIKMR 1615
PF-028 ALDCSEQSVILWYETILDKIVGVIK 1616
PRP PF-C031 WSESQPPTATPRPHAEVARAGLVTPPTL 1617
PF-752 LHVIRPRPELSELKFPITKILKVNKQGLKK 1618
PF-672 MRFGSLALVAYDSAIKHSWPRPSSVRRLRM 1619
PF-088 VMFVLTRGRSPRPMIPAY 1620
PF-143 LSPRPIIVSRRSRADNNNDWSR 1621
PF-168 VLPFPAIPLSRRRACVAAPRPRSRQRAS 1622
PF-531 YIQFHLNQQPRPKVKKIKIFL 1623
All groups are associated with antimicrobial activity
In certain embodiments, peptides described herein can have multiple activities. Thus for example, a peptide can have both binding/targeting activity and antimicrobial activity. Illustrative peptides having multiple activities are shown in Table 8. Such peptides can be used, e.g., in a chimeric construct, for any or all of these properties. Thus, for example, a peptide designated “B” in Table 8 can be used as a targeting peptide. If it is also designated G or M it can also be used for antimicrobial activity.
TABLE 8
Peptides having multiple activities.
Peptide Activities
PF-001 G B
PF-002 G B
PF-003 G B
PF-004 G B
PF-005 G B
PF-006 G B M
PF-007 G B
PF-008 G B
PF-009 G B
PF-010 G B
PF-011 G B
PF-012 G B
PF-013 G B
PF-015 G B
PF-017 G B
PF-020 G B
PF-021 G B
PF-022 G B
PF-023 G B
PF-024 G B
PF-025 G B
PF-026 G B
PF-027 G B
PF-028 G B
PF-029 G B
PF-030 G B
PF-031 G B
PF-033 G B
PF-034 G B
PF-035 G B
PF-036 G B
PF-037 G B
PF-040 G B
PF-041 G B
PF-042 G B
PF-043 G B
PF-045 G B
PF-046 G B
PF-048 G B
PF-049 G B
PF-051 G B
PF-052 G B
PF-053 G B
PF-056 G B
PF-057 G B
PF-058 G B
PF-061 G B
PF-063 G B
PF-064 G B
PF-065 G B
PF-066 G B
PF-067 G B
PF-068 G B
PF-069 G B
PF-070 G B
PF-071 G B
PF-073 G B
PF-074 G B
PF-075 G B
PF-076 G B
PF-099 G B
PF-123 G B
PF-124 G B
PF-125 G B
PF-127 G B
PF-128 G B
PF-129 G B
PF-133 G B
PF-135 G B
PF-137 G B
PF-139 G B
PF-140 G B
PF-143 G B
PF-144 G B
PF-145 G B
PF-148 G B M
PF-149 G B
PF-153 G B
PF-156 G B
PF-157 G B
PF-164 G B
PF-168 G B M
PF-171 G B
PF-173 G B
PF-175 G B
PF-176 G B
PF-178 G B
PF-180 G B
PF-186 G B
PF-188 G B
PF-190 G B
PF-191 G B
PF-192 G B
PF-196 G B
PF-203 G B
PF-204 G B
PF-208 G B
PF-209 G B M
PF-212 G B
PF-215 G B
PF-224 G B
PF-226 G B
PF-233 G B
PF-234 G B
PF-235 G B
PF-249 G B
PF-255 G B
PF-257 G B
PF-270 G B
PF-271 G B
PF-273 G B
PF-276 G B
PF-278 G B M
PF-283 G B M
PF-289 G B
PF-292 G B
PF-294 G B
PF-297 G B
PF-301 G B
PF-305 G B
PF-306 G B
PF-307 G B M
PF-313 G B
PF-319 G B
PF-322 G M
PF-344 G B
PF-347 G B
PF-349 G B
PF-350 G B
PF-354 G B
PF-355 G B
PF-356 G B
PF-357 G B
PF-360 G B
PF-362 G B
PF-363 G B
PF-366 G B
PF-369 G B
PF-370 G B
PF-373 G B
PF-374 G B
PF-375 G B
PF-376 G B
PF-378 G B
PF-379 G B
PF-380 G B
PF-381 G B
PF-382 G B
PF-383 G B
PF-385 G B
PF-386 G B
PF-387 G B
PF-389 G B
PF-390 G B
PF-392 G B
PF-393 G B
PF-394 G B
PF-395 G B
PF-396 G B
PF-397 G B
PF-398 G B
PF-399 G B
PF-401 G B
PF-403 G B
PF-404 G B
PF-405 G B
PF-406 G B
PF-407 G B
PF-408 G B
PF-410 G B
PF-411 G B
PF-413 G B
PF-414 G B
PF-416 G B
PF-417 G B
PF-418 G B
PF-421 G B
PF-422 G B
PF-423 G B
PF-424 G B
PF-425 G B
PF-426 G B
PF-427 G B
PF-428 G B
PF-429 G B
PF-430 G B
PF-431 G B
PF-432 G B
PF-433 G B
PF-434 G B
PF-437 G M
PF-439 G B
PF-440 G B
PF-442 G B
PF-443 G B
PF-444 G B
PF-445 G B
PF-446 G B
PF-447 G B
PF-S003 G B
PF-448 G B M
PF-450 G B
PF-451 G B
PF-452 G B
PF-453 G B
PF-454 G B
PF-456 G B
PF-457 G B
PF-458 G B
PF-459 G B
PF-460 G B
PF-461 G B
PF-462 G B
PF-464 G B
PF-465 G B
PF-466 G B
PF-467 G B
PF-469 G B
PF-470 G B
PF-471 G B
PF-472 G B
PF-473 G B
PF-474 G B
PF-475 G B
PF-476 G B
PF-477 G B
PF-478 G B
PF-479 G B
PF-480 G B
PF-482 G B
PF-484 G B
PF-497 B M
PF-499 B M
PF-511 G B M
PF-512 G B M
PF-513 G B
PF-514 G B
PF-515 G B
PF-516 G
PF-517 G B
PF-518 G B
PF-519 G B
PF-520 G B M
PF-521 G B M
PF-522 G B M
PF-523 B M
PF-524 G B M
PF-525 G M
PF-526 G B
PF-527 G B M
PF-528 G B
PF-529 G B M
PF-530 G M
PF-531 G M
PF-537 G B
PF-538 G M
PF-539 G B
PF-540 G B
PF-542 G B
PF-543 G B
PF-544 G B
PF-545 G B M
PF-546 G B
PF-547 G B M
PF-548 G B
PF-549 G B
PF-550 G B
PF-551 G B
PF-552 G B
PF-553 G B
PF-554 G B
PF-555 G B
PF-556 G B
PF-557 G B
PF-558 G B
PF-559 G B
PF-560 G B
PF-562 G B
PF-563 G B
PF-564 G B
PF-566 G B
PF-567 G B
PF-569 G B
PF-572 G B
PF-573 G B
PF-575 G B
PF-576 G B
PF-577 G B
PF-578 G B
PF-580 G B
PF-581 G B
PF-583 G B M
PF-584 G B
PF-585 G B
PF-586 G B
PF-587 G B
PF-588 G B
PF-589 G B
PF-590 G B
PF-592 G B
PF-593 G B
PF-594 G B
PF-595 G B
PF-596 G B
PF-597 G B
PF-598 G B
PF-599 G B
PF-600 G B M
PF-601 G B
PF-602 G B
PF-603 G B
PF-604 G B
PF-605 G B
PF-606 G M
PF-607 G B
PF-609 G B
PF-610 G B
PF-612 G B
PF-613 G B
PF-614 G B
PF-615 G B
PF-616 G B
PF-617 G B
PF-619 G B
PF-621 G B
PF-622 G B
PF-623 G B
PF-625 G B
PF-626 G B
PF-627 G B
PF-629 G B
PF-630 G B
PF-631 G B
PF-632 G B
PF-634 G B
PF-635 G B
PF-636 G B
PF-637 G B
PF-638 G B
PF-639 G B
PF-640 G B
PF-642 G B
PF-655 G B
PF-664 G B
PF-672 G B M
PF-681 G B
PF-686 G B
PF-737 G B
PF-738 G B
PF-741 G B
PF-744 G B
PF-745 G B
PF-746 G B
PF-748 G B
PF-749 G B
PF-752 G B
PF-756 G B
PF-757 G B
PF-760 G B
PF-761 G B
PF-762 G B
PF-763 G B
PF-764 G B
PF-770 G B
PF-776 G B
PF-C052 G B
PF-C055 G B
PF-C057 G B
PF-C058 G B
PF-C061 G B
PF-C062 G B
PF-C064 G B
PF-C065 G B
PF-C069 G B
PF-C071 G B
PF-C072 G B
PF-C075 G B
PF-C084 G B
PF-C085 G B
PF-C086 G B
PF-C088 G B
PF-C091 G B
PF-C095 G B
PF-C098 G B
PF-C120 G B
PF-C131 G B
PF-C135 G B
PF-C136 G B
PF-C137 G B
PF-C139 G B
PF-C142 G B
PF-C143 G B
PF-C145 G B
PF-C180 G B
PF-C181 G B
PF-C194 G B
PF-C281 G B
PF-C290 G B
PF-C291 G B
B: targeting/binding activity;
M: antimicrobial activity;
G: Growth or phenotype altering.
Other peptides believed to show binding, growth altering, and/or antimicrobial activity are shown in Table 9.
TABLE 9
Additional peptides believed to have binding,
growth altering, and/or antimicrobial activity.
ID Sequence SEQ ID No.
PF-198 RRLASRRSLVVST 1624
PF-227 RLLGLYGENSAAGFIASVIGAVIILFIYNLIARKS 1625
PF-260 GHLRVCWILWLQSANPLSFRHHYLAVMW 1626
PF-261 MDIWKFIKSFNTVNTYLLLSCVLLIILVLYFYVINPA 1627
PF-277 MIIQNKKIEKIYKYQTKEIFLNKTSLRAGFVFRMVRVLI 1628
PF-280 MLIDWQEPDIEKSFCAAFLKISVSVLVYRTPLGYGNQLRE 1629
PF-286 FFDGEVGCGC 1630
PF-287 ILEQNIEEVFFIQS 1631
PF-312 MDKIRIWNNFHISNEYIKQRYGIISIPLFYVYLF 1632
PF-321 FAKKNPCRMRVPNTGTWYLVVNQDGNSGIVNFSINTIQN 1633
PF-327 MLVFQMRYQMRYVDKTSTVLKQTKNSDYADK 1634
PF-330 MLMNFEVYQQRILIIYNKCYHLKAVGKNLQLFIIVD 1635
PF-331 MGRHLWNPSYFVATVSENTEEQIRKYINNQKKQVK 1636
PF-341 DDKNEGKIAQGEY 1637
PF-391 EASVYRE 1638
PF-420 MVKHNFDVTDKTGKISSKHCFEITDKTDVV 1639
PF-708 DRPSQTTHHTLSSSRITGPS 1640
PF-710 EALLPPDPPDEDSQRIIPQ 1641
PF-713 DRPSQTTHHTLSSSRITGPS 1642
PF-715 LEDTKALFPCFVPI 1643
PF-718 KKYSSFKSMIDDLEYDA 1644
PF-719 FKSMIDDLEYDA 1645
PF-721 TEQAKKIVDILNNWLE 1646
PF-722 STSPSVTSVYAEALGLK 1647
PF-723 VGAMAIFLNVVAMLAGV 1648
PF-725 ARTIQNNGCLIHNSRYP 1649
PF-726 CDDLYALEAQGTLNELLKK 1650
PF-729 TPEPVVIVKP 1651
PF-730 FEDIEQIIKYHLIDGKIVAPLLLDR 1652
PF-734 SDIIAEMFQQGELEPMLRDAVAA 1653
PF-736 KGSASGSASGSGSAK 1654
PF-739 KSGASSVASAAKSG 1655
PF-742 AAATTATTAK 1656
PF-743 TKGTTTGTAKTTGVTTGTAK 1657
PF-769 GSRGGAKRGGARG 1658
PF- WSESQPPTATPRPHAEVARAGLVTPPTL 1659
C031
PF- QPIGFPTDSVHGTDLVHRLRGTTSSR 1660
C038
PF- LENLDIEGLTEMKEHIEDLIAEKSAAESIEEVIVEAE 1661
C077
PF- AYSLTFQNPNDNLTDEEVAKYMEKITKALTEKIGAEVR 1662
C205
PF-S016 PLTRETFAERGIRKARVARTFSEEEPPF 1663
III. Design and Construction of STAMPs and Other Chimeric Constructs. In various embodiments this invention provides chimeric moieties comprising one or more targeting moieties attached to one or more effectors. The targeting moieties can be selected to preferentially bind to a target microorganism (e.g., bacteria, virus, fungi, yeast, alga, protozoan, etc.) or group of microorganisms (e.g., gram-negative or gram-positive bacteria, particular genus, species, etc.) In certain embodiments the targeting moiety comprises one or more novel microorganism-binding peptides as described herein (see, e.g., Table 3, and/or Table 10, and/or Table 12). In certain embodiments the targeting moiety comprises non-peptide moieties (e.g., antibodies, receptor, receptor ligand, lectin, and the like).
In various embodiments the effector comprises a moiety whose activity is to be delivered to the target microorganism(s), to a biofilm comprising the target microorganism(s), to a cell or tissue comprising the target microorganism(s), and the like. In certain embodiments the targeting moiety comprises one or more antimicrobial peptide(s) as described herein (see, e.g., Tables 4, 5 and/or 14), an antibiotic (including, but not limited to a steroid antibiotic), a detectable label, a porphyrin, a photosensitizing agent, an epitope tag, a lipid or liposome, a nanoparticle, a dendrimer, and the like.
In certain embodiments one or more targeting moieties are attached to a single effector. In certain embodiments one or more effectors are attached to a single targeting moiety. In certain embodiments multiple targeting moieties are attached to multiple effectors. The targeting moieties(s) can be attached directly to the effector(s) or through a linker. Where the targeting moiety and the effector comprise peptides the chimeric moiety can be a fusion protein.
A) Targeting Moieties.
In various embodiments this invention provides targeting moieties that preferentially and/or specifically bind to a microorganism (e.g., a bacterium, a fungus, a yeast, etc.). One or more such targeting moieties can be attached to one or more effectors to provide chimeric moieties that are capable of delivering the effector(s) to a target (e.g., a bacterium, a fungus, a yeast, a biofilm comprising the bacterium or fungus or yeast, etc.).
In various embodiments, targeting moieties include, but are not limited to peptides that preferentially bind particular microorganisms (e.g., bacteria, fungi, yeasts, protozoa, algae, viruses, etc.) or groups of such microorganisms, e.g., as described above, antibodies that bind particular microorganisms or groups of microorganisms, receptor ligands that bind particular microorganisms or groups of microorganisms, porphyrins (e.g., metalloporphyrins), lectins that bind particular microorganisms or groups of microorganisms, and the like. As indicated it will be appreciated that references to microorganisms or groups of microorganism include bacteria or groups of bacteria, viruses or groups of viruses, yeasts or groups of yeasts, protozoa or groups of protozoa, viruses or groups of viruses, and the like.
i. Targeting Peptides.
In certain embodiments, the targeting moiety comprises one or more targeting peptides that bind particular bacteria, fungi, and/or yeasts, and/or algae, and/or viruses and/or that bind particular groups of bacteria, and/or groups of fungi, and/or groups of yeasts, and/or groups of algae.
In certain embodiments the targeting peptide can comprise one or more domains capable of binding, specifically binding, or preferentially binding to a microorganism, e.g., a target microbial organism (see, e.g., Table 3). In certain embodiment, the targeting peptide be identified via screening peptide libraries. For example, a phage display peptide library can be screened against a target microbial organism or a desired antigen or epitope thereof. Any peptide identified through such screening can be used as a targeting peptide for the target microbial organism. Illustrative additional targeting peptides are shown in Table 10.
TABLE 10
Additional illustrative targeting moieties.
SEQ
Targeting Moiety/ ID
Organism Structure/sequence NO
LPSB-1 RGLRRLGRRGLRRLGR 1664
Phob-1 KPVLPVLPVLPVL 1665
LPSB-2 VLRIIRIAVLRIIRIA 1666
LPTG-1 LPETGGSGGSLPETG 1667
α-1 RAHIRRAHIRR 1668
ANION-1 DEDEDDEEDDDEEE 1669
PHILIC-1 STMCGSTMCGSTMCG 1670
SA5.1/S. aureus VRLPLWLPSLNE 1671
SA5.3/S. aureus ANYFLPPVLSSS 1672
SA5.4/S. aureus SHPWNAQRELSV 1673
SA5.5/S. aureus SVSVGMRPMPRP 1674
SA5.6/S. aureus WTPLHPSTNRPP 1675
SA5.7/S. aureus SVSVGMKPSPRP 1676
SA5.8/S. aureus SVSVGMKPSPRP 1677
SA5.9/S. aureus SVPVGPYNESQP 1678
SA5.10/S. aureus WAPPLFRSSLFY 1679
SA2.2/S. aureus WAPPXPXSSLFY 1680
SA2.4/S. aureus HHGWTHHWPPPP 1681
SA2.5/S. aureus SYYSLPPIFHIP 1682
SA2.6/S. aureus HFQENPLSRGGEL 1683
SA2.7/S. aureus FSYSPTRAPLNM 1684
SA2.8/S. aureus SXPXXMKXSXXX 1685
SA2.9/S. aureus VSRHQSWHPHDL 1686
SA2.10/S. aureus DYXYRGLPRXET 1687
SA2.11/S. aureus SVSVGMKPSPRP 1688
S. aureus/Consensus V/Q/H-P/H-H-E-F/Y-K/H-H/A-L/H-X-X-K/R-P/L 1689
DH5.1/E coli. KHLQNRSTGYET 1690
DH5.2/E coli. HIHSLSPSKTWP 1691
DH5.3/E coli. TITPTDAEMPFL 1692
DH5.4/E coli. HLLESGVLERGM 1693
DH5.5/E coli. HDRYHIPPLQLH 1694
DH5.6/E coli. VNTLQNVRHMAA 1695
DH5.7/E coli. SNYMKLRAVSPF 1696
DH5.8/E coli. NLQMPYAWRTEF 1697
DH5.9/E coli. QKPLTGPHFSLI 1698
CSP/S. mutans SGSLSTFFRLFNRSFTQALGK 1699
CSPC18/S. mutans LSTFFRLFNRSFTQALGK 1700
CSPC16/S. mutans TFFRLFNRSFTQALGK 1701
CSPM8/S. mutans TFFRLFNR 1702
KH/Pseudomonas spp KKHRKHRKHRKH 1703
(US 2004/0137482)
cCF10 LVTLVFV 1704
AgrD1 YSTCDFIM 1705
AgrD2 GVNACSSLF 1706
AgrD3 YINCDFLL 1707
NisinA ITSISLCTPGCKTGALMGCNMRTATCIICSIIIVSK 1708
PlnA KSSAYSLQMGATAIKQVKKLFKKWGW 1709
S3L1-5 WWYNWWQDW 1710
Penetratin RQIKIWFWNRRMKWKK* 1711
Tat EHWSYCDLRPG 1712
Pep-1N KETWWETWWTEW 1713
Pep27 MRKEFHNVLSSGQLLADKRPARDYNRK 1714
HABP35 LKQKIKHVVKLKVVVKLRSQLVKRKQN 1715
HABP42 (all D) STMMSRSHKTRSHHV 1716
HABP52 GAHWQFNALTVRGGGS 1717
Hi3/17 KQRTSIRATEGCLPS 1718
α-E. coli peptide QEKIRVRLSA 1719
Salivary Receptor QLKTADLPAGRDETTSFVLV* 1720
Adhesion Fragment
S1 (Sushi frag.) GFKLKGMARISCLPNGQWSNFPPKCIRECAMVSS 1721
(LPS binding)
S3 (Sushi frag.) HAEHKVKIGVEQKYGQFPQGTEVTYTCSGNYFLM 1722
(LPS binding)
MArg.1 AMDMYSIEDRYFGGYAPEVG 1723
(Mycoplasma infected
cell line binding
peptide
BPI fragment 1 ASQQGTAALQKELKRIKPDYSDSFKIKH 1724
(LPS binding)
6,376,462
BPI fragment 2 SSQISMVPNVGLKFSISNANIKISGKWKAQKRFLK 1725
(LPS binding)
6,376,462
BPI fragment 3 VHVHISKSKVGWLIQLFHKKIESALRNK 1726
(LPS binding)
6,376,462
LBP fragment 1 AAQEGLLALQSELLRITLPDFTGDLRIPH 1727
(LPS binding)
6,376,462
LBP fragment 2 HSALRPVPGQGLSLSISDSSIRVQGRWKVRKSFFK 1728
(LPS binding)
6,376,462
LBP fragment 3 VEVDMSGDLGWLLNLFHNQIESKFQKV 1729
(LPS binding)
6,376,462
B. anthracis spore ATYPLPIR 1730
binding
(WO/1999/036081)
Bacillus spore binding peptides of 5-12 amino acids containing the sequence 1731
(WO/1999/036081) Asn-His-Phe-Leu
peptides of 5-12 amino acids containing the sequence 1732
Asn-His-Phe-Leu-Pro
Thr-Ser-Glu-Asn-Val-Arg-Thr (TSQNVRT) 1733
A peptide of formula Thr-Tyr-Pro-X-Pro-X-Arg 1734
(TYPXPXR) where X is a Ile, Val or Leu.
A peptide having the sequence TSQNVRT. 1735
A peptide having the sequence TYPLPIR 1736
LPS binding peptide 1 TFRRLKWK 1737
(6,384,188)
LPS BP 2 (6,384,188) RWKVRKSFFKLQ 1738
LPS BP 3 (6,384,188) KWKAQKRFLKMS 1739
Pseudomonas pilin KCTSDQDEQFIPKGCSK 1740
binding peptide
(5,494,672)
RNAII inhibiting YSPWTNF 1741
peptide (S. Aureus)
Patents and patent publications disclosing the referenced antibodies are identified in the table.
In certain embodiments the targeting moieties can comprise other entities, particularly when utilized with an antimicrobial peptide as described, for example, in Table 4. Illustrative targeting moieties can include a polypeptide, a peptide, a small molecule, a ligand, a receptor, an antibody, a protein, or portions thereof that specifically interact with a target microbial organism, e.g., the cell surface appendages such as flagella and pili, and surface exposed proteins, lipids and polysaccharides of a target microbial organism.
ii. Targeting Antibodies.
In certain embodiments the targeting moieties can comprise one or more antibodies that bind specifically or preferentially a microorganism or group of microorganisms (e.g., bacteria, fungi, yeasts, protozoa, viruses, algae, etc.). The antibodies are selected to bind an epitope characteristic or the particular target microorganism(s). In various embodiments such epitopes or antigens are typically is gram-positive or gram-negative specific, or genus-specific, or species-specific, or strain specific and located on the surface of a target microbial organism. The antibody that binds the epitope or antigen can direct an anti-microbial peptide moiety or other effector to the site. Furthermore, in certain embodiments the antibody itself can provide anti-microbial activity in addition to the activity provided by effector moiety since the antibody may engage an immune system effector (e.g., a T-cell) and thereby elicit an antibody-associated immune response, e.g., a humoral immune response.
Antibodies that bind particular target microorganisms can be made using any methods readily available to one skilled in the art. For example, as described in U.S. Pat. No. 6,231,857 (incorporated herein by reference) three monoclonal antibodies, i.e., SWLA1, SWLA2, and SWLA3 have been made against S. mutans. Monoclonal antibodies obtained from non-human animals to be used in a targeting moiety can also be humanized by any means available in the art to decrease their immunogenicity and increase their ability to elicit anti-microbial immune response of a human. Illustrative microorganisms and/or targets to which antibodies may be directed are shown, for example, in Tables 3 and 11.
Various forms of antibody include, without limitation, whole antibodies, antibody fragments (e.g., (Fab′)2 Fab′, etc.), single chain antibodies (e.g., scFv), minibodies, Di-miniantibody, Tetra-miniantibody, (scFv)2, Diabody, scDiabody, Triabody, Tetrabody, Tandem diabody, VHH, nanobodies, affibodies, unibodies, and the like.
Methods of making such antibodies are well known to those of skill in the art. In various embodiments, such methods typically involve providing the microorganism, or a component thereof for use as an antigen to raise an immune response in an organism or for use in a screening protocol (e.g., phage or yeast display).
For example, polyclonal antibodies are typically raised by one or more injections (e.g. subcutaneous or intramuscular injections) of the target microorganism(s) or components thereof into a suitable non-human mammal (e.g., mouse, rabbit, rat, etc.).
If desired, the immunizing microorganism or antigen derived therefrom can be administered with or coupled to a carrier protein by conjugation using techniques that are well-known in the art. Such commonly used carriers which are chemically coupled to the peptide include keyhole limpet hemocyanin (KLH), thyroglobulin, bovine serum albumin (BSA), and tetanus toxoid. The coupled peptide is then used to immunize the animal (e.g. a mouse or a rabbit).
The antibodies are then obtained from blood samples taken from the mammal. The techniques used to develop polyclonal antibodies are known in the art (see, e.g., Methods of Enzymology, “Production of Antisera With Small Doses of Immunogen: Multiple Intradermal Injections”, Langone, et al. eds. (Acad. Press, 1981)). Polyclonal antibodies produced by the animals can be further purified, for example, by binding to and elution from a matrix to which the peptide to which the antibodies were raised is bound. Those of skill in the art will know of various techniques common in the immunology arts for purification and/or concentration of polyclonal antibodies, as well as monoclonal antibodies see, for example, Coligan, et al. (1991) Unit 9, Current Protocols in Immunology, Wiley Interscience).
In certain embodiments the antibodies produced will be monoclonal antibodies (“mAb's”). The general method used for production of hybridomas secreting mAbs is well known (Kohler and Milstein (1975) Nature, 256:495
Antibody fragments, e.g. single chain antibodies (scFv or others), can also be produced/selected using phage display and/or yeast display technology. The ability to express antibody fragments on the surface of viruses that infect bacteria (bacteriophage or phage) or yeasts makes it possible to isolate a single binding antibody fragment, e.g., from a library of greater than 1010 nonbinding clones. To express antibody fragments on the surface of phage (phage display) or yeast, an antibody fragment gene is inserted into the gene encoding a phage surface protein (e.g., pIII) and the antibody fragment-pIII fusion protein is displayed on the phage surface (McCafferty et al. (1990) Nature, 348: 552-554; Hoogenboom et al. (1991) Nucleic Acids Res. 19: 4133-4137).
Since the antibody fragments on the surface of the phage or yeast are functional, phage bearing antigen binding antibody fragments can be separated from non-binding phage by antigen affinity chromatography (McCafferty et al. (1990) Nature, 348: 552-554). Depending on the affinity of the antibody fragment, enrichment factors of 20 fold -1,000,000 fold are obtained for a single round of affinity selection.
Human antibodies can be produced without prior immunization by displaying very large and diverse V-gene repertoires on phage (Marks et al. (1991) J. Mol. Biol. 222: 581-597.
In certain embodiments, nanobodies can be used as targeting moieties. Methods of making VhH (nanobodies) are also well known to those of skill in the art. The Camelidae heavy chain antibodies are found as homodimers of a single heavy chain, dimerized via their constant regions. The variable domains of these camelidae heavy chain antibodies are referred to as VHH domains or VHH, and can be either used per se as nanobodies and/or as a starting point for obtaining nanobodies. Isolated VHH retain the ability to bind antigen with high specificity (see, e.g., Hamers-Casterman et al. (1993) Nature 363: 446-448). In certain embodiments such VHH domains, or nucleotide sequences encoding them, can be derived from antibodies raised in Camelidae species, for example in camel, dromedary, llama, alpaca and guanaco. Other species besides Camelidae (e.g. shark, pufferfish) can produce functional antigen-binding heavy chain antibodies, from which (nucleotide sequences encoding) such naturally occurring VHH can be obtained, e.g. using the methods described in U.S. Patent Publication US 2006/0211088.
In various embodiments, for use in therapy, human proteins are preferred, primarily because they are not as likely to provoke an immune response when administered to a patient. Comparisons of camelid VHH with the VH domains of human antibodies reveals several key differences in the framework regions of the camelid VHH domain corresponding to the VH/VL interface of the human VH domains. Mutation of these human residues to VHH resembling residues has been performed to produce “camelized” human VH domains that retain antigen binding activity, yet have improved expression and solubility.
Libraries of single VH domains have also been derived for example from VH genes amplified from genomic DNA or from mRNA from the spleens of immunized mice and expressed in E. coli (Ward et al. (1989) Nature 341: 544-546) and similar approaches can be performed using the VH domains and/or the VL domains described herein. The isolated single VH domains are called “dAbs” or domain antibodies. A “dAb” is an antibody single variable domain (VH or VL) polypeptide that specifically binds antigen. A “dAb” binds antigen independently of other V domains; however, as the term is used herein, a “dAb” can be present in a homo- or heteromultimer with other VH or VL domains where the other domains are not required for antigen binding by the dAb, i.e., where the dAb binds antigen independently of the additional VH or VL domains.
As described in U.S. Patent Publication US 2006/0211088 methods are known for the cloning and direct screening of immunoglobulin sequences (including but not limited to multivalent polypeptides comprising: two or more variable domains—or antigen binding domains—and in particular VH domains or VHH domains; fragments of VL, VH or VHH domains, such as CDR regions, for example CDR3 regions; antigen-binding fragments of conventional 4-chain antibodies such as Fab fragments and scFv's, heavy chain antibodies and domain antibodies; and in particular of VH sequences, and more in particular of VHH sequences) that can be used as part of and/or to construct such nanobodies.
Methods and procedures for the production of VHH/nanobodies can also be found for example in WO 94/04678, WO 96/34103, WO 97/49805, WO 97/49805 WO 94/25591, WO 00/43507 WO 01/90190, WO 03/025020, WO 04/062551, WO 04/041863, WO 04/041865, WO 04/041862, WO 04/041867, PCT/BE2004/000159, Hamers-Casterman et al. (1993) Nature 363: 446; Riechmann and Muyldermans (1999) J. Immunological Meth., 231: 25-38; Vu et al. (1997) Molecular Immunology, 34(16-17): 1121-1131; Nguyen et al. (2000) EMBO J., 19(5): 921-930; Arbabi Ghahroudi et al. (19997) FEBS Letters 414: 521-526; van der Linden et al. (2000) J. Immunological Meth., 240: 185-195; Muyldermans (2001) Rev. Molecular Biotechnology 74: 277-302; Nguyen et al. (2001) Adv. Immunol. 79: 261, and the like.
In certain embodiments the antibody targeting moiety is a unibody. Unibodies provide an antibody technology that produces a stable, smaller antibody format with an anticipated longer therapeutic window than certain small antibody formats. In certain embodiments unibodies are produced from IgG4 antibodies by eliminating the hinge region of the antibody. Unlike the full size IgG4 antibody, the half molecule fragment is very stable and is termed a uniBody. Halving the IgG4 molecule left only one area on the UniBody that can bind to a target. Methods of producing unibodies are described in detail in PCT Publication WO2007/059782, which is incorporated herein by reference in its entirety (see, also, Kolfschoten et al. (2007) Science 317: 1554-1557).
Affibody molecules are class of affinity proteins based on a 58-amino acid residue protein domain, derived from one of the IgG-binding domains of staphylococcal protein A. This three helix bundle domain has been used as a scaffold for the construction of combinatorial phagemid libraries, from which Affibody variants that target the desired molecules can be selected using phage display technology (see, e.g,. Nord et al. (1997) Nat. Biotechnol. 15: 772-777; Ronmark et al. (2002) Eur. J. Biochem., 269: 2647-2655.). Details of Affibodies and methods of production are known to those of skill (see, e.g., U.S. Pat. No 5,831,012 which is incorporated herein by reference in its entirety).
It will also be recognized that antibodies can be prepared by any of a number of commercial services (e.g., Berkeley antibody laboratories, Bethyl Laboratories, Anawa, Eurogenetec, etc.).
Illustrative antibodies that bind various microorganisms are shown in Table 11.
TABLE 11
Illustrative antibodies that bind target microorganisms.
Source Antibody
U.S. Pat. No. 7,195,763 Polyclonal/monoclonal binds specific
Gram(+) cell wall repeats
U.S. Pat. No. 6,939,543 Antibodies against G(+) LTA
U.S. Pat. No. 7,169,903 Antibodies against G(+) peptidoglycan
U.S. Pat. No. 6,231,857 Antibody against S. mutans (Shi)
U.S. Pat. No. 5,484,591 Gram(−) binding antibodies
US 2007/0231321 Diabody binding to Streptococcus
surface antigen I/II
US 2003/0124635 Antibody against S. mutans
US 2006/0127372 Antibodies to Actinomyces naeslundii,
Lactobacillus casei
US 2003/0092086 Antibody to S. sobrinus
U.S. Pat. No. 7,364,738 Monoclonal antibodies to the ClfA protein
in S. aureus
U.S. Pat. No. 7,632,502 Antibodies against C. albicans
U.S. Pat. No. 7,608,265 Monoclonal against C. difficile
U.S. Pat. No. 4,777,136 Monoclonal Antibodies against
Pseudomonas aeruginosa
see, e.g., ab20429, ab20560, Antibody against S. pneumoniae
ab79522, ab35165, ab65602
from AbCAMm Cambridge
Science Park, U.K.
In addition, antibodies (targeting moieties) that bind other microorganisms can readily be produced using, for example, the methods described above.
iii. Porphyrins.
In certain embodiments porphyrins, or other photosensitizing agents, can be used as targeting moieties in the constructs described herein. In particular, metalloporphyrins, particularly a number of non-iron metalloporphyrins mimic heme in their molecular structure and are actively accumulated by bacteria via high affinity heme-uptake systems. The same uptake systems can be used to deliver antibiotic-porphyrin and antibacterial-porphyrin conjugates. Illustrative targeting porphyrins suitable for this purpose are described in U.S. Pat. No. 6,066,628 and shown herein, for example, in FIGS. 1 and 2.
For example, certain artificial (non-iron) metalloporphyrins (MPs) (Ga-IX, Mn-IX,) are active against Gram-negative and Gram-positive bacteria and acid-fast bacilli (e.g., Y. enterocolitica, N. meningitides, S. marcescens, E. coli, P. mirabills, K. pneumoniae, K. oxytoca, Ps. aeruginosa, C. freundii, E. aerogenes, F. menigosepticum, S. aureus, B. subtilis, S. pyogenes A, E. faecalis, M smegmatis, M bovis, M tuber., S. crevisiae) as described in Tables 1-5 of U.S. Pat. No. 6,066,628. These MPs can be used as targeting moieties against these microorganisms.
Similarly, some MPs are also growth-inhibitory against yeasts, indicating their usefulness targeting moieties to target Candida species (e.g., Candida albicans, C. krusei, C. pillosus, C. glabrata, etc.) and other mycoses including but not limited to those caused by as Trichophyton, Epidermophyton, Histoplasma, Aspergillus, Cryptococcus, and the like.
Porphyrins, and other photosensitizers, also have antimicrobial activity. Accordingly, in certain embodiments, the porphyrins, or other photosensitizers, can be used as effectors (e.g., attached to targeting peptides as described herein). In various embodiments the porphyrins or other photosensitizers can provide a dual functionality, e.g., as a targeting moiety and an antimicrobial and can be attached to a targeting peptide and/or to an antimicrobial peptide as described herein.
Illustrative porphyrins and other photosensitizers are shown in FIGS. 1-11 and described in more detail in the discussion of effectors below.
iv. Pheromones.
In certain embodiments, pheromones from microorganisms can be used as targeting moieties. Illustrative pheromones from bacteria and fungi are shown in Table 12.
TABLE 12
Illustrative bacterial and fungal pheromones utilizable as targeting moieties.
Bacterial Pheromones
Locus tag Product Sequence SEQ ID
gi|1041118|dbj|BAA11198.1| iPD1 [Enterococcus MKQQKKHIAALLF 1742
faecalis] ALILTLVS
gi|1113947|gb|AAB35253.1| iAM373sex pheromone SIFTLVA 1743
inhibito [Enterococcus
faecalis, Peptide, 7 aa]
gi|115412|sp|P13268.1|CAD1_ENTFA Sex pheromone CAD1 LFSLVLAG 1744
gi|116406|sp|P11932.1|CIA_ENTFA Sex pheromone cAM373 AIFILAS 1745
(Clumping-inducing
agent) (CIA)
gi|117240|sp|P13269.1|CPD1_ENTFA Sex pheromone cPD1 FLVMFLSG 1746
gi|12056953|gb|AAG48144.1|AF322594_1 putative peptide DSIRDVSPTFNKIRR 1747
pheromone PrcA WFDGLFK
[Lactobacillus paracasei]
gi|123988|sp|P24803.1|IAD1_ENTFA Sex pheromone inhibitor MSKRAMKKIIPLIT 1748
determinant precursor LFVVTLVG
(iAD1)
gi|126362994|emb|CAM35812.1| precursor of pheromone KDEIYWKPS 1749
peptide ComX [Bacillus
amyloliquefaciens FZB42]
gi|1587088|prf||2205353A pheromone YSTCDFIM 1750
gi|15900442|ref|NP_345046.1| peptide pheromone BlpC GLWEDLLYNINRY 1751
[Streptococcus AHYIT
pneumoniae TIGR4]
gi|1617436|emb|CAA66791.1| competence pheromone DIRHRINNSIWRDIF 1752
[Streptococcus gordonii] LKRK
gi|1617440|emb|CAA66786.1| competence pheromone DVRSNKIRLWWEN 1753
[Streptococcus gordonii] IFFNKK
gi|18307870|gb|AAL67728.1|AF456134_2 ComX pheromone PTTREWDG 1754
precursor [Bacillus
mojavensis]
gi|18307874|gb|AAL67731.1|AF456135_2 ComX pheromone LQIYTNGNWVPS 1755
precursor [Bacillus
mojavensis]
gi|29377808|ref|NP_816936.1| sex pheromone inhibitor MSKRAMKKIIPLIT 1756
determinant [Enterococcus LFVVTLVG
faecalis V583]
gi|3342125|gb|AAC27522.1| putative pheromone GAGKNLIYGMGYG 1757
[Enterococcus faecium] YLRSCNRL
gi|41018893|sp|P60242.1|CSP1_STRPN Competence-stimulating EMRLSKFFRDFILQ 1758
peptide type 1 precursor RKK
(CSP-1)
gi|57489126|gb|AAW51333.1| PcfP [Enterococcus WSEIEINTKQSN 1759
faecalis]
gi|57489152|gb|AAW51349.1| PrgT [Enterococcus HISKERFEAY 1760
faecalis]
gi|58616083|ref|YP_195761.1| UvaF [Enterococcus KYKCSWCKRVYTL 1761
faecalis] RKDHRTAR
gi|58616111|ref|YP_195802.1| PcfP [Enterococcus WSEIEINTKQSN 1762
faecalis]
gi|58616132|ref|YP_195769.1| PrgQ [Enterococcus MKTTLKKLSRYIA 1763
faecalis] VVIAITLIFI
gi|58616137|ref|YP_195772.1| PrgT [Enterococcus HISKERFEAY 1764
faecalis]
gi|6919848|sp|O33689.1|CSP_STROR Competence-stimulating DKRLPYFFKHLFSN 1765
peptide precursor (CSP) RTK
gi|6919849|sp|O33666.1|CSP2_STRMT Competence-stimulating EMRKPDGALFNLF 1766
peptide precursor (CSP) RRR
gi|6919850|sp|O33668.1|CSP3_STRMT Competence-stimulating EMRKSNNNFFHFL 1767
peptide precursor (CSP) RRI
gi|6919851|sp|O33672.1|CSP1_STRMT Competence-stimulating ESRLPKIRFDFIFPR 1768
peptide precursor (CSP) KK
gi|6919852|sp|O33675.1|CSP4_STRMT Competence-stimulating EIRQTHNIFFNFFKRR 1769
peptide precursor (CSP)
gi|6919853|sp|O33690.1|CSP2_STROR Competence-stimulating DWRISETIRNLIFPR 1770
peptide precursor (CSP) RK
gi|999344|gb|AAB34501.1| cOB1bacterial sex VAVLVLGA 1771
pheromone [Enterococcus
faecalis, Peptide, 8 aa]
gi|18307878|gb|AAL67734.1|AF456136_2 ComX pheromone FFEDDKRKSFI 1772
precursor [Bacillus
subtilis]
gi|18307882|gb|AAL67737.1|AF456137_2 ComX pheromone FFEDDKRKSFI 1773
precursor [Bacillus
subtilis]
gi|28272731|emb|CAD65660.1| accessory gene regulator MKQKMYEAIAHLF 1774
protein D, peptide KYVGAKQLVMCC
pheromone precursor VGIWFETKIPDELRK
[Lactobacillus plantarum
WCFS1]
gi|28379890|ref|NP_786782.1| accessory gene regulator MKQKMYEAIAHLF 1775
protein D, peptide KYVGAKQLVMCC
pheromone precursor VGIWFETKIPDELRK
[Lactobacillus plantarum
WCFS1]
gi|57489105|gb|AAW51312.1| PrgF [Enterococcus VVAYVITQVGAIRF 1776
faecalis]
gi|58616090|ref|YP_195779.1| PrgF [Enterococcus VVAYVITQVGAIRF 1777
faecalis]
gi|58616138|ref|YP_195762.1| PrgN [Enterococcus LLKLQDDYLLHLE 1778
faecalis] RHRRTKKIIDEN
gi|57489117|gb|AAW51324.1| PcfF [Enterococcus EDIKDLTDKVQSLN 1779
faecalis] ALVQSELNKLIKRK
DQS
gi|57489119|gb|AAW51326.1| PcfH [Enterococcus WFLDFSDWLSKVP 1780
faecalis] SKLWAE
gi|58616102|ref|YP_195792.1| PcfF [Enterococcus EDIKDLTDKVQSLN 1781
faecalis] ALVQSELNKLIKRK
DQS
gi|58616104|ref|YP_195794.1| PcfH [Enterococcus WFLDFSDWLSKVP 1782
faecalis] SKLWAE
Fungi
gi|1127585|gb|AAA99765.1| mfa1 gene product MLSIFAQTTQTSAS 1783
EPQQSPTAPQGRDN
GSPIGYSSCVVA
gi|1127592|gb|AAA99771.1| mfa2 gene product MLSIFETVAAAAPV 1784
TVAETQQASNNEN
RGQPGYYCLIA
gi|11907715|gb|AAG41298.1| pheromone precursor PSLPSSPPSLLPPLPL 1785
MFalpha1D LKLLATRRPTLVG
[Cryptococcus neoformans MTLCV
var. neoformans]
gi|13810235|emb|CAC37424.1| M-factor precursor Mfm1 MDSMANSVSSSSV 1786
[Schizosaccharomyces VNAGNKPAETLNK
pombe] TVKNYTPKVPYMC
VIA
gi|14269436|gb|AAK58071.1|AF378295_1 peptide mating pheromone MDTFTYVDLAAVA 1787
precursor Bbp2-3 AAAVADEVPRDFE
[Schizophyllum DQITDYQSYCIIC
commune]
gi|14269440|gb|AAK58073.1|AF378297_1 peptide mating pheromone SNVHGWCVVA 1788
precursor Bbp2-1
[Schizophyllum
commune]
gi|1813600|gb|AAB41859.1| pheromone precursor NTTAHGWCVVA 1789
Bbp1(1) [Schizophyllum
commune]
gi|24940428|emb|CAD56313.1| a-pheromone MQPSTVTAAPKDK 1790
[Saccharomyces TSAEKKDNYIIKGV
paradoxus] FWDPACVIA
gi|27549492|gb|AAO17258.1| pheromone phb3.1 GPTWWCVNA 1791
[Coprinopsis cinerea]
gi|27549494|gb|AAO17259.1| pheromone phb3.2 SGPTWFCIIQ 1792
[Coprinopsis cinerea]
gi|27752314|gb|AAO19469.1| pheromone protein a FTAIFSTLSSSVASK 1793
pecursor [Cryptococcus TDAPRNEEAYSSG
neoformans var. grubii] NSP
gi|2865510|gb|AAC02682.1| MAT-1 pheromone MFSIFAQPAQTSVS 1794
[Ustilago hordei] ETQESPANHGANP
GKSGSGLGYSTCV
VA
gi|3023372|sp|P78742.1|BB11_SCHCO RecName: Full = Mating- NTTAHGWCVVA 1795
type pheromone BBP1(1);
Flags: Precursor
gi|3025079|sp|P56508.1|SNA2_YEAST RecName: Full = Protein SDDNYGSLA 1796
SNA2
gi|37626077|gb|AAQ96360.1| pheromone precursor Phb3 NGLTFWCVIA 1797
B5 [Coprinopsis cinerea]
gi|37626081|gb|AAQ96362.1| pheromone precursor PSWFCVIA 1798
Phb3.2 B45 [Coprinopsis
cinerea]
gi|37626083|gb|AAQ96363.1| pheromone precursor ASWFCTIA 1799
Phb3.1 B47 [Coprinopsis
cinerea]
gi|37961432|gb|AAP57503.1| Ste3-like pheromone PHHKIANASDKRR 1800
receptor [Thanatephorus RMYFEIFMCAVL
cucumeris]
gi|400250|sp|P31962.1|MFA1_USTMA RecName: Full = A1- MLSIFAQTTQTSAS 1801
specific pheromone; EPQQSPTAPQGRDN
AltName: Full = Mating GSPIGYSSCVVA
factor A1
gi|400251|sp|P31963.1|MFA2_USTMA RecName: Full = A2- MLSIFETVAAAAPV 1802
specific pheromone; TVAETQQASNNEN
AltName: Full = Mating RGQPGYYCLIA
factor A2
gi|41209131|gb|AAR99617.1| lipopeptide mating SLTYAWCVVA 1803
pheromone precursor
Bap2(3) [Schizophyllum
commune]
gi|41209146|gb|AAR99650.1| lipopeptide mating TSMAHAWCVVA 1804
pheromone precursor
Bap3(2) [Schizophyllum
commune]
gi|41209149|gb|AAR99653.1| lipopeptide mating GYCVVA 1805
pheromone precursor
Bbp2(8) [Schizophyllum
commune]
gi|46098187|gb|EAK83420.1| MFA1_USTMA A1- MLSIFAQTTQTSAS 1806
SPECIFIC PHEROMONE EPQQSPTAPQGRDN
(MATING FACTOR A1) GSPIGYSSCVVA
[Ustilago maydis 521]
gi|546861|gb|AAB30833.1| M-factor mating MDSMANTVSSSVV 1807
pheromone NTGNKPSETLNKT
[Schizosaccharomyces VKNYTPKVPYMCV
pombe] IA
gi|5917793|gb|AAD56043.1|AF184069_1 pheromone Mfa2 MFSLFETVAAAVK 1808
[Ustilago hordei] VVSAAEPEHAPTNE
GKGEPAPYCIIA
gi|6014618|gb|AAF01424.1|AF186389_1 Phb3.2.42 [Coprinus LTWFCVIA 1809
cinereus]
gi|68266363|gb|AAY88882.1| putative pheromone LREKRRRRWFEAF 1810
receptor STE3.4 MGFGL
[Coprinellus disseminatus]
gi|71012805|ref|XP_758529.1| A1-specific pheromone MLSIFAQTTQTSAS 1811
[Ustilago maydis 521] EPQQSPTAPQGRDN
GSPIGYSSCVVA
gi|72414834|emb|CAI59748.1| mating factor a1.3 MDALTLFAPVSLG 1812
[Sporisorium reilianum] AVATEQAPVDEER
PNRQTFPWIGCVVA
gi|72414854|emb|CAI59758.1| mating factor a2.1 MFIFESVVASVQAV 1813
[Sporisorium reilianum] SVAEQDQTPVSEG
RGKPAVYCTIA
gi|1127587|gb|AAA99767.1| rba1 gene product PWMSLLFSFLALLA 1814
LILPKLSKDDPLGL
TRQPR
gi|151941959|gb|EDN60315.1| pheromone-regulated ASISLIMEGSANIEA 1815
membrane protein VGKLVWLAAALPL
[Saccharomyces cerevisiae AFI
YJM789]
gi|3025095|sp|Q07549.1|SNA4_YEAST Protein SNA4 ARNVYPSVETPLLQ 1816
GAAPHDNKQSLVE
SPPPYVP
gi|73921293|sp|Q08245.3|ZEO1_YEAST RecName: Full = Protein FLKKLNRKIASIFN 1817
ZEO1; AltName:
Full = Zeocin resistance
protein 1
gi|74644573|sp|Q9P305.3|IGO2_YEAST RecName: Full = Protein DSISRQGSISSGPPP 1818
EDF (E. coli) IGO2 RSPNK
NNWNN 1819
v. Targeting Enhancers/Opsonins
In certain embodiments compositions are contemplated that incorporate a targeting enhancer (e.g., an opsonin) along with one or more targeting moieties (e.g., targeting peptides). Targeting enhancers include moieties that increase binding affinity, and/or binding specificity, and/or internalization of a moiety by the target cell/microorganism.
Accordingly, in certain embodiments, a targeting moiety and/or a targeted antimicrobial molecule comprise a peptide, with the desired level of binding specificity and/or avidity, attached (e.g., conjugated) to an opsonin. When bound to a target cell through the targeting peptide, the opsonin component encourages phagocytosis and destruction by resident macrophages, dendritic cells, monocytes, or PMNs. Opsonins contemplated for conjugation can be of a direct or indirect type.
Direct opsonins include, fore example, any bacterial surface antigen, PAMP (pathogen-associated molecular pattern), or other molecule recognized by host PRRs (pathogen recognizing receptors). Opsonins can include, but are not limited to, bacterial protein, lipid, nucleic acid, charbohydrate and/or oligosaccharide moieties.
In certain embodiments opsonins include, but are not limited to, N-acetyl-D-glucosamine (GlcNAc), N-acetyl-D-galactosamine (GlaNAc), N-acetylglucosamine-containing muramyl peptides, NAG-muramyl peptides, NAG-NAM, peptidoglycan, teichoic acid, lipoteichoic acid, LPS, o-antigen, mannose, fucose, ManNAc, galactose, maltose, glucose, glucosamine, sucrose, mannosamine, galactose-alpha-1,3-galactosyl-beta-1,4-N-acetyl glucosamine, or alpha-1,3-gal-gal, or other sugars.
In certain embodiments, opsonins include indirect opsonins. Indirect opsonins function through binding to a direct opsonin already present. For example an Fc portion of an antibody, a sugar-binding lectin protein (example MBL), or host complement factors (example C3b, C4b, iC3b).
In certain embodiments the opsonin is to galactose-alpha-1,3-galactosyl-beta-1,4-N-acetyl glucosamine, or alpha1,3-gal-gal.
Other examples of opsonin molecules include, but are not limited to antibodies (e.g., IgG and IgA), components of the complement system (e.g., C3b, C4b, and iC3b), mannose-binding lectin (MBL) (initiates the formation of C3b), and the like.
Methods of coupling an opsonin to a targeting moiety are well known to those of skill in the art (see, e.g., discussion below regarding attachment of effectors to targeting moieties).
B) Effectors.
Any of a wide number of effectors can be coupled to targeting moieties as described herein to preferentially deliver the effector to a target organism and/or tissue. Illustrative effectors include, but are not limited to detectable labels, small molecule antibiotics, antimicrobial peptides, porphyrins or other photosensitizers, epitope tags/antibodies for use in a pretargeting protocol, agents that physically disrupt the extracellular matrix within a community of microorganisms, microparticles and/or microcapsules, nanoparticles and/or nanocapsules, “carrier” vehicles including, but not limited to lipids, liposomes, dendrimers, cholic acid-based peptide mimics or other peptide mimics, steroid antibiotics, and the like.
i. Detectable labels.
In certain embodiments chimeric moieties are provided comprising a targeting moiety (e.g., as described in Table 3) attached directly or through a linker to a detectable label. Such chimeric moieties are effective for detecting the presence and/or quantity, and/or location of the microorganism(s) to which the targeting moiety is directed. Similarly these chimeric moieties are useful to identify cells and/or tissues and/or food stuffs and/or other compositions that are infected with the targeted microorganism(s).
Detectable labels suitable for use in such chimeric moieties include any composition detectable by spectroscopic, photochemical, biochemical, immunochemical, electrical, optical, or chemical means. Illustrative useful labels include, but are not limited to, biotin for staining with labeled streptavidin conjugates, avidin or streptavidin for labeling with biotin conjugates fluorescent dyes (e.g., fluorescein, texas red, rhodamine, green fluorescent protein, and the like, see, e.g., Molecular Probes, Eugene, Oreg., USA), radiolabels (e.g.,3H, 125I, 35S, 14C, 32P, 99Tc, 203Pb, 67Ga, 68Ga, 72As, 111In, 113mIn, 97Ru, 62Cu, 641Cu, 52Fe, 52mMn, 51Cr, 186Re, 188Re, 77As, 90Y, 67Cu, 169Er, 121Sn, 127Te, 142Pr, 143Pr, 198Au, 199Au, 161Tb, 109Pd, 165Dy, 149Pm, 151Pm, 153Sm, 157Gd, 159Gd, 166Ho, 172Tm, 169Yb, 175Yb, 177Lu, 105Rh, 111Ag, and the like), enzymes (e.g. horse radish peroxidase, alkaline phosphatase and others commonly used in an ELISA), various colorimetric labels, magnetic or paramagnetic labels (e.g., magnetic and/or paramagnetic nanoparticles), spin labels, radio-opaque labels, and the like. Patents teaching the use of such labels include, for example, U.S. Pat. Nos. 3,817,837; 3,850,752; 3,939,350; 3,996,345; 4,277,437; 4,275,149; and 4,366,241.
It will be recognized that fluorescent labels are not to be limited to single species organic molecules, but include inorganic molecules, multi-molecular mixtures of organic and/or inorganic molecules, crystals, heteropolymers, and the like. Thus, for example, CdSe-CdS core-shell nanocrystals enclosed in a silica shell can be easily derivatized for coupling to a biological molecule (Bruchez et al. (1998) Science, 281: 2013-2016). Similarly, highly fluorescent quantum dots (zinc sulfide-capped cadmium selenide) have been covalently coupled to biomolecules for use in ultrasensitive biological detection (Warren and Nie (1998) Science, 281: 2016-2018).
In various embodiments spin labels are provided by reporter molecules with an unpaired electron spin which can be detected by electron spin resonance (ESR) spectroscopy. Illustrative spin labels include organic free radicals, transitional metal complexes, particularly vanadium, copper, iron, and manganese, and the like. Exemplary spin labels include, for example, nitroxide free radicals.
Means of detecting such labels are well known to those of skill in the art. Thus, for example, where the label is a radioactive label, means for detection include a scintillation counter or photographic film as in autoradiography. Where the label is a fluorescent label, it may be detected by exciting the fluorochrome with the appropriate wavelength of light and detecting the resulting fluorescence, e.g., by microscopy, visual inspection, via photographic film, by the use of electronic detectors such as charge coupled devices (CCDs) or photomultipliers and the like. Similarly, enzymatic labels may be detected by providing appropriate substrates for the enzyme and detecting the resulting reaction product. Finally, simple colorimetric labels may be detected simply by observing the color associated with the label.
ii. Antibiotics.
In certain embodiments chimeric moieties are provided comprising a targeting moiety (e.g. as described in Table 3) attached directly or through a linker to a small molecule antibiotic and/or to a carrier (e.g., a lipid or liposome, a polymer, etc.) comprising a small molecule antibiotic. Illustrative antibiotics are shown in Table 13.
TABLE 13
Illustrative antibiotics for use in the chimeric moieties described herein.
Class Generic Name BRAND NAME
Aminoglycosides Amikacin AMIKIN ®
Gentamicin GARAMYCIN ®
Kanamycin KANTREX ®
Neomycin
Netilmicin NETROMYCIN ®
Streptomycin
Tobramycin NEBCIN ®
Paromomycin HUMATIN ®
Carbacephem Loracarbef LORABID ®
Carbapenems Ertapenem INVANZ ®
Doripenem FINIBAX ®
Imipenem/Cilastatin PRIMAXIN ®
Meropenem MERREM ®
Cephalosporins Cefadroxil DURICEF ®
(First generation) Cefazolin ANCEF ®
Cefalotin or Cefalothin KEFLIN ®
Cefalexin KEFLEX ®
Cephalosporins Cefaclor CECLOR ®
(Second Cefamandole MANDOLE ®
generation) Cefoxitin MEFOXIN ®
Cefprozil CEFZIL ®
Cefuroxime CEFTIN, ZINNAT ®
Cephalosporins Cefixime SUPRAX ®
(Third Cefdinir OMNICEF ®
generation) Cefditoren SPECTRACEF ®
Cefoperazone CEFOBID ®
Cefotaxime CLAFORAN ®
Cefpodoxime
Ceftazidime FORTAZ ®
Ceftibuten CEDAX ®
Ceftizoxime
Ceftriaxone ROCEPHIN ®
Cephalosporins Cefepime MAXIPIME ®
(Fourth
generation)
Cephalosporins Ceftobiprole
(Fifth generation)
Glycopeptides Teicoplanin
Vancomycin VANCOCIN ®
Macrolides
Azithromycin Zithromax
Clarithromycin Biaxin
Dirithromycin
Erythromycin Erythocin, Erythroped
Roxithromycin
Troleandomycin
Telithromycin Ketek
Monobactams
Aztreonam
Penicillins Amoxicillin NOVAMOX ®, AMOXIL ®
Ampicillin
Azlocillin
Carbenicillin
Cloxacillin
Dicloxacillin
Flucloxacillin FLOXAPEN ®
Mezlocillin
Meticillin
Nafcillin
Oxacillin
Penicillin
Piperacillin
Ticarcillin
Polypeptides Bacitracin
Colistin
Polymyxin B
Quinolones Mafenide
Prontosil (archaic)
Sulfacetamide
Sulfamethizole
Sulfanilimide (archaic)
Sulfasalazine
Sulfisoxazole
Trimethoprim BACTRIM ®
Trimethoprim-
Sulfamethoxazole (Co-
trimoxazole)
(TMP-SMX)
Tetracyclines Demeclocycline
Doxycycline VIBRAMYCIN ®
Minocycline MINOCIN ®
Oxytetracycline TERRACIN ®
Tetracycline SUMYCIN ®
Natural products Antimicrobial herbal
extracts
Essential oils
Farnesol
Licorice root extracts
Glycyrrhizol A
Glycyrrhizol B
6,8-diisoprenyl-5,7,4′-
trihydroxyisoflavone
Others Arsphenamine SALVARSAN ®
Chloramphenicol CHLOROMYCETIN ®
Clindamycin CLEOCIN ®
Lincomycin
Ethambutol
Fosfomycin
Fusidic acid FUCIDIN ®
Furazolidone
Isoniazid
Linezolid ZYVOX ®
Metronidazole FLAGYL ®
Mupirocin BACTROBAN ®
Nitrofurantoin MACRODANTIN ®,
MACROBID ®
Platensimycin
Pyrazinamide
Quinupristin/ SYNCERCID ®
Dalfopristin
Rifampin or
Rifampicin
Tinidazole
Artemisinin
Antifungals Amphotericin B
Anidulafungin
Caspofungin acetate
Clotrimazole
Fluconazole
Flucytosine
Griseofulvin
Itraconazole
Ketoconazole
Micafungin
Miconazole
Nystatin
Pentamidine
Posaconazole
Terbinafine
Voriconazole
Antimycobiotics Aminosalicylic Acid
Capreomycin
Clofazimine
Cycloserine
Ethionamide
Rifabutin
Rifapentine
Antivirals Abacavir
Acyclovir
Adefovir
Amantadine
Atazanavir
Cidofovir
Darunavir
Didanosine
Docosanol
Efavirenz
Emtricitabine
Enfuvirtide
Entecavir
Etravirine
Famciclovir
Fomivirsen
Fosamprenavir
Foscarnet
Ganciclovir
Idoxuridine
Indinavir
Interferon alpha
Lamivudine
Lopinavir/ritonavir
Maraviroc
Nelfinavir
Nevirapine
Oseltamivir
Penciclovir
Peramivir
Raltegravir
Ribavirin
Rimantadine
Ritonavir
Saquinavir
Stavudine
Telbivudine
Tenofovir
Tipranavir
Trifluridine
Valacyclovir
Valganciclovir
Zanamivir
Zidovudine
Anti-parasitics Albendazole
Artesunate
Atovaquone
Bephenium
hydroxynaphthoate
Chloroquine
Dapsone
Diethyl-carbamazine
Diloxanide furoate
Eflornithine
Emetine HCl
Furazolidone
Ivermectin
Lindane
Mebendazole
Mefloquine
Melarsoprol
Miltefosine
Niclosamide
Nifurtimox
Nitazoxanide
Oxamniquine
Paromomycin
Permethrin
Piperazine
Praziquantel
Primaquine
Pyrantel pamoate
Pyrimethamine
Proguanil
Quinacrine HCl
Quinidine
Quinine
Sodium Stibogluconate
Spiramycin
Thiabendazole
Tinidazole
iii. Porphyrins and Non-Porphyrin Photosensitizers.
In certain embodiments, porphyrins and other photosensitizers can be used as targeting moieties and/or as effectors in the methods and compositions of this invention. A photosensitizer is a drug or other chemical that increases photosensitivity of the organism (e.g., bacterium, yeast, fungus, etc.). As targeting moieties the photosensitizers (e.g., porphyrins) are preferentially uptaken by the target microorganisms and thereby facilitate delivery of the chimeric moiety to the target microorganism.
As effectors, photosensitizers can be useful in photodynamic antimicrobial chemotherapy (PACT). In various embodiments PACT utilizes photosensitizers and light (e.g., visible, ultraviolet, infrared, etc.) in order to give a phototoxic response in the target organism(s), often via oxidative damage.
Currently, the major use of PACT is in the disinfection of blood products, particularly for viral inactivation, although more clinically-based protocols are used, e.g. in the treatment of oral infection or topical infection. The technique has been shown to be effective in vitro against bacteria (including drug-resistant strains), yeasts, viruses, parasites, and the like.
Attaching a targeting moiety (e.g., a targeting peptide) to the photosensitizer, e.g., as described herein, provides a means of specifically or preferentially targeting the photosensitizer(s) to particular species or strains(s) of microorganism.
A wide range of photosensitizers, both natural and synthetic are known to those of skill in the art (see, e.g., Wainwright (1998) J. Antimicrob. Chemotherap. 42: 13-28). Photosensitizers are available with differing physicochemical make-up and light-absorption properties. In various embodiments photosensitizers are usually aromatic molecules that are efficient in the formation of long-lived triplet excited states. In terms of the energy absorbed by the aromatic-system, this again depends on the molecular structure involved. For example: furocoumarin photosensitizers (psoralens) absorb relatively high energy ultraviolet (UV) light (c. 300-350 nm), whereas macrocyclic, heteroaromatic molecules such as the phthalocyanines absorb lower energy, near-infrared light.
Illustrative photosensitizers include, but are not limited to porphyrinic macrocyles (especially porphyrins, chlorines, etc., see, e.g., FIGS. 1 and 2). In particular, metalloporphyrins, particularly a number of non-iron metalloporphyrins mimic haem in their molecular structure and are actively accumulated by bacteria via high affinity haem-uptake systems. The same uptake systems can be used to deliver antibiotic-porphyrin and antibacterial-porphyrin conjugates. Illustrative targeting porphyrins suitable for this purpose are described in U.S. Pat. No. 6,066,628 and shown herein in FIGS. 1 and 2.
Illustrative examples of targeted porphyrins are described in Example 5 and associated figures and in FIG. 13.
For example, certain artificial (non-iron) metalloporphyrins (MPs) (Ga-IX, Mn-IX,) are active against Gram-negative and Gram-positive bacteria and acid-fast bacilli (e.g., Y. enterocolitica, N. meningitides, S. marcescens, E. coli, P. mirabills, K. pneumoniae, K. oxytoca, Ps. aeruginosa, C. freundii, E. aerogenes, F. menigosepticum, S. aureus, B. subtilis, S. pyogenes A, E. faecalis, M smegmatis, M bovis, M tuber., S. crevisiae) as described in Tables 1-5 of U.S. Pat. No. 6,066,628. These MPs can be used as targeting moieties against these microorganisms.
Similarly, some MPs are also growth-inhibitory against yeasts, indicating their usefulness targeting moieties to target Candida species (e.g., Candida albicans, C. krusei, C. pillosus, C. glabrata, etc.) and other mycoses including but not limited to those caused by as Trichophyton, Epidermophyton, Histoplasma, Aspergillus, Cryptococcus, and the like.
Other photosensitizers include, but are not limited to cyanines (see, e.g,. FIG. 6) and phthalocyanines (see, e.g., FIG. 4), azines (see, e.g., FIG. 5) including especially methylene blue and touidine blue, hypericin (see, e.g., FIG. 8), acridines (see, e.g., FIG. 9) including especially Rose Bengal (see, e.g., FIG. 10), crown ethers (see, e.g., FIG. 11), and the like. In certain embodiments, the photosensitizers include tin chlorin 6 and related compounds (e.g., other chlorines and tin porphyrins).
Another light-activated compound is cucumin (see, FIG. 12).
In certain embodiments the photosensitizers are toxic or growth inhibitors without light activation. For example, some non-iron metalloporphyrins (MPs) (see, e.g., FIGS. 1 and 2 herein) possess a powerful light-independent antimicrobial activity. In addition, haemin, the most well known natural porphyrin, possesses a significant antibacterial activity that can augmented by the presence of physiological concentrations of hydrogen peroxide or a reducing agent.
Typically, when activated by light, the toxicity or growth inhibition effect is substantially increased. Typically, they generate radical species that affect anything within proximity. In certain embodiments to get the best selectivity from targeted photosensitizers, anti-oxidants can be used to quench un-bound photosensitizers, limiting the damage only to cells where the conjugates have accumulated due to the targeting peptide. The membrane structures of the target cell act as the proton donors in this case.
In typical photodynamic antimicrobial chemotherapy (PACT) the targeted photosensitizer is “activated by the application of a light source (e.g., a visible light source, an ultraviolate light source, an infrared light source, etc.). PACT applications however need not be limited to topical use. Regions of the mouth, throat, nose, sinuses are readily illuminated. Similarly regions of the gut can readily be illuminated using endoscopic techniques. Other internal regions can be illumined using laparoscopic methods or during other surgical procedures. For example, in certain embodiments involving the insertion or repair or replacement of an implantable device (e.g., a prosthetic device) it contemplated that the device can be coated or otherwise contacted with a chimeric moiety comprising a targeting moiety attached to a photosensitizer as described herein. During the surgical procedure and/or just before closing, the device can be illuminated with an appropriate light source to activate the photosensitizer.
The targeted photosensitizers and uses thereof described herein are illustrative and not to be limiting. Using the teachings provided herein, other targeted photosensitizers and uses thereof will be available to one of skill in the art.
iv. Antimicrobial Peptides.
In certain embodiments, the effector can comprise one or more antimicrobial peptides or compound antimicrobial peptides, e.g., as described above. Numerous antimicrobial peptides are well known to those of skill in the art.
In certain embodiments the antimicrobial peptides comprise one or more amino acid sequences described above (e.g., one or more domains comprising amino acid sequences in Tables 4 and/or 5) and/or one or more of the amino acid sequences shown in Table 14. In certain embodiments the antimicrobial peptides comprise one or more amino acid sequences described in the “Collection of Anti-Microbial Peptides” (CAMP) an online database developed for advancement the understanding of antimicrobial peptides (see, e.g., Thomas et al. (2009) Nucleic Acids Research, 2009, 1-7.doi:10.1093/nar/gkp1021) available at www.bicnirrh.res.in/antimicrobial.
TABLE 14
Other illustrative antimicrobial peptides. AP numbers refer to ID in
antimicrobial peptide database (http://aps.unmc.edu/AP/main.php).
SEQ
ID
Effector Structure/Sequence No
AP00274 1BH4, Circulin A GIPCGESCVWIPCISAALGCSCKNK 1820
(CirA, plant VCYRN
cyclotides, XXC,
ZZHp)
AP00036 1BNB, Beta- DFASCHTNGGICLPNRCPGHMIQIG 1821
defensin 1 (cow) ICFRPRVKCCRSW
AP00047 1BNB, Bovine GPLSCGRNGGVCIPIRCPVPMRQIG 1822
neutrophil beta- TCFGRPVKCCRSW
defensin 12
(BNBD-12, cow)
AP00428 1C01, MiAMP1 SAFTVWSGPGCNNRAERYSKCGCS 1823
(Macadamia AIHQKGGYDFSYTGQTAALYNQA
integrifolia GCSGVAHTRFGSSARACNPFGWKS
antimicrobial IFIQC
peptide 1, plant)
AP00154 1CIX, Tachystatin YSRCQLQGFNCVVRSYGLPTIPCC 1824
A2 (Horseshoe RGLTCRSYFPGSTYGRCQRY
crabs, Crustacea,
BBS)
AP00145 1CW5, VNYGNGVSCSKTKCSVNWGQAFQ 1825
Carnobacteriocin ERYTAGINSFVSGVASGAGSIGRRP
B2 (CnbB2, class
IIA
bacteriocin, bacteria)
AP00153 1CZ6, Androctonin RSVCRQIKICRRRGGCYYKCTNRPY 1826
(scorpions)
AP00152 1D6X, Tritrpticin VRRFPWWWPFLRR 1827
(synthetic)
AP00201 1D7N, Mastoparan INLKALAALAKKIL 1828
(insect)
AP00140 1D9J, CecropinA- KWKLFKKIGIGKFLHSAKKF 1829
Magainin2 hybrid
(synthetic)
AP00178 1DFN, human DCYCRIPACIAGERRYGTCIYQGRL 1830
alpha Defensin WAFCC
HNP-3 (human
neutrophil peptide-
3, HNP3, human
defensin, ZZHh)
AP01153 1DQC, Tachycitin YLAFRCGRYSPCLDDGPNVNLYSC 1831
(horseshoe crabs, CSFYNCHKCLARLENCPKGLHYN
Crustacea, BBS) AYLKVCDWPSKAGCT
AP00437 1DUM, Magainin 2 GIGKYLHSAKKFGKAWVGEIMNS 1832
analog (synthetic)
AP00451 1E4S, Human beta DHYNCVSSGGQCLYSACPIFTKIQG 1833
defensin 1 (HBD-1, TCYRGKAKCCK
human defensin)
AP00149 1EWS, Rabbit MPCSCKKYCDPWEVIDGSCGLFNS 1834
kidney defensin 1 KYICCREK
(RK-1)
AP00141 1F0E, CecropinA- KWKLFKKIPKFLHSAKKF 1835
Magainin2 Hybrid
(P18, synthetic)
AP00142 1F0G, CecropinA- KLKLFKKIGIGKFLHSAKKF 1836
Magainin2 Hybrid
(synthetic)
AP00143 1F0H, CecropinA- KAKLFKKIGIGKFLHSAKKF 1837
Magainin2 Hybrid
(synthetic)
AP00524 1FD4, Human beta GIGDPVTCLKSGAICHPVFCPRRYK 1838
defensin 2 (HBD-2, QIGTCGLPGTKCCKKP
human defensin,
ZZHh)
AP00438 1FJN, Mussel GFGCPNNYQCHRHCKSIPGRCGGY 1839
Defensin MGD-1 CGGWHRLPCTCYRCG
AP00155 1FRY, SMAP-29 RGLRRLGRKIAHGVKKYGPTVLRII 1840
(SMAP29, sheep RIAG
cathelicidin)
AP00150 1G89, Indolicidin ILPWKWPWWPWRR 1841
(cow cathelicidin,
BBN, ZZHa)
AP00156 1GR4, Microcin VGIGTPISFYGGGAGHVPEYF 1842
J25, linear
(MccJ25,
bacteriocin,
bacteria)
AP00151 1HR1, Indolicidin ILAWKWAWWAWRR 1843
P to A mutant
(synthetic)
AP00196 1HU5, Ovispirin-1 KNLRRIIRKIIHIIKKYG 1844
(synthetic)
AP00197 1HU6, Novispirin KNLRRIIRKGIHIIKKYG 1845
G10 (synthetic)
AP00198 1HU7, Novispirin KNLRRITRKIIHIIKKYG 1846
T7 (synthetic)
AP00445 1HVZ, Monkey GFCRCLCRRGVCRCICTR 1847
RTD-1 (rhesus
theta-defensin-1,
minidefensin-1,
animal defensin,
XXC, BBS, lectin,
ZZHa)
AP00103 1i2v, Heliomicin DKLIGSCVWGAVNYTSDCNGECL 1848
variant (Hel-LL, LRGYKGGHCGSFANVNCWCET
synthetic)
AP00216 1ICA, Phormia ATCDLLSGTGINHSACAAHCLLRG 1849
defensin A (insect NRGGYCNGKGVCVCRN
defensin A)
AP01224 1Jo3, Gramicidin B VGALAVVVWLFLWLW 1850
(bacteria)
AP01225 1jo4, Gramicidin C VGALAVVVWLYLWLW 1851
(bacteria)
AP00191 1KFP, Gomesin ECRRLCYKQRCVTYCRGR 1852
(Gm, Spider, XXA)
AP00283 1KJ6, Huamn beta GIINTLQKYYCRVRGGRCAVLSCL 1853
defensin 3 (HBD-3, PKEEQIGKCSTRGRKCCRRKK
human defensin,
ZZHh)
AP00147 1KV4, Moricin AKIPIKAIKTVGKAVGKGLRAINIA 1854
(insect, silk moth) STANDVFNFLKPKKRKA
AP00227 1L4V, Sapecin ATCDLLSGTGINHSACAAHCLLRG 1855
(insect, flesh fly) NRGGYCNGKAVCVCRN
AP01161 1L9L, Human GRDYRTCLTIVQKLKKMVDKPTQ 1856
granulysin RSVSNAATRVCTRGRSRWRDVCR
(huGran) NFMRRYQSRVIQGLVAGETAQQIC
EDLRLCIPSTGPL
AP00026 1LFC, FKCRRWQWRMKKLGAPSITCVRR 1857
Lactoferricin B AF
(LfcinB, cow,
ZZHa)
AP00193 1M4F, human DTHFPICIFCCGCCHRSKCGMCCKT 1858
LEAP-1 (Hepcidin
25)
AP00499 1MAG, Gramicidin VGALAVVVWLWLWLW 1859
A (gA, bacteria)
AP00403 1MM0, Termicin ACNFQSCWATCQAQHSIYFRRAFC 1860
(termite defensin, DRSQCKCVFVRG
insect defensin)
AP00194 1MMC, Ac-AMP2 VGECVRGRCPSGMCCSQFGYCGK 1861
(plant defensin, GPKYCGR
BBS)
AP01206 1MQZ, Mersacidin CTFTLPGGGGVCTLTSECIC 1862
(bacteria)
AP00429 1NKL, Porcine GYFCESCRKIIQKLEDMVGPQPNE 1863
NK-Lysin (pig) DTVTQAASQVCDKLKILRGLCKKI
MRSFLRRISWDILTGKKPQAICVDI
KICKE
AP00633 1og7, Sakacin P/ KYYGNGVHCGKHSCTVDWGTAIG 1864
Sakacin 674 (SakP, NIGNNAAANWATGGNAGWNK
class IIA
bacteriocin,
bacteria)
AP00195 1PG1, Protegrin 1 RGGRLCYCRRRFCVCVGR 1865
(Protegrin-1, PG-1,
pig cathelicidin,
XXA, ZZHa,
BBBm)
AP00928 1PXQ, Subtilosin NKGCATCSIGAACLVDGPIPDFEIA 1866
A (XXC, class I GATGLFGLWG
bacteriocin, Gram-
positive bacteria)
AP00480 1Q71, Microcin VGIGTPIFSYGGGAGHVPEYF 1867
J25 (cyclic
MccJ25, class I
microcins,
bacteriocins, Gram-
negative bacteria,
XXC; BBP)
AP00211 1RKK, RRWCFRVCYRGFCYRKCR 1868
Polyphemusin I
(crabs, Crustacea)
AP00430 1T51, IsCT ILGKIWEGIKSLF 1869
(Scorpion)
AP00731 1ut3, Spheniscin-2 SFGLCRLRRGFCARGRCRFPSIPIGR 1870
(Sphe-2, penguin CSRFVQCCRRVW
defensin, avian
defensin)
AP00013 1VM5, Aurein 1.2 GLFDIIKKIAESF 1871
(frog)
AP00214 1WO1, KWCFRVCYRGICYRRCR 1872
Tachyplesin I
(crabs, Crustacea,
XXA, ZZHa)
AP00644 1xc0, Pardaxin 4 GFFALIPKIISSPLFKTLLSAVGSALS 1873
(Pardaxin P-4, SSGGQE
Pardaxin P4, Pa4,
flat fish)
AP00493 1XKM, Distinctin NLVSGLIEARKYLEQLHRKLKNCKV 1874
(two chains for
stability and
transport? frog)
AP00420 1XV3, Penaeidin- HSSGYTRPLRKPSRPIFIRPIGCDVC 1875
4d (penaeidin 4, YGIPSSTARLCCFRYGDCCHL
shrimp, Crustacea)
AP00035 1YTR, Plantaricin KSSAYSLQMGATAIKQVKKLFKK 1876
A (PlnA, WGW
bacteriocin,
bacteria)
AP00166 1Z64, Pleurocidin GWGSFFKKAAHVGKHVGKAALT 1877
(fish) HYL
AP00780 1Z6V, Human GRRRRSVQWCAVSQPEATKCFQW 1878
lactoferricin QRNMRKVRGPPVSCIKRDSPIQCIQA
AP00549 1ZFU, Plectasin GFGCNGPWDEDDMQCHNHCKSIK 1879
(fungi, fungal GYKGGYCAKGGFVCKCY
defensin)
AP00177 1ZMH, human CYCRIPACIAGERRYGTCIYQGRL 1880
alpha Defensin WAFCC
HNP-2 (human
neutrophil peptide-
2, HNP2, human
defensin, ZZHh)
AP00179 1ZMM, human VCSCRLVFCRRTELRVGNCLIGGV 1881
alpha Defensin SFTYCCTRVD
HNP-4 (human
neutrophil peptide-
4, HNP4, human
defensin)
AP00180 1ZMP, human QARATCYCRTGRCATRESLSGVCE 1882
alpha Defensin ISGRLYRLCCR
HD-5 (HD5,
human defensin)
AP00181 1ZMQ, human STRAFTCHCRRSCYSTEYSYGTCT 1883
alpha Defensin VMGINHRFCCL
HD-6 (HD6,
human defensin)
AP00399 1ZRW, Spinigerin HVDKKVADKVLLLKQLRIMRLLT 1884
(insect, termite) RL
AP01157 1ZRX, Stomoxyn RGFRKHFNKLVKKVKHTISETAHV 1885
(insect) AKDTAVIAGSGAAVVAAT
AP00637 2A2B, Curvacin A/ ARSYGNGVYCNNKKCWVNRGEA 1886
sakacin A (CurA, TQSIIGGMISGWASGLAGM
SakA, class IIA
bacteriocin,
bacteria)
AP00558 2B68, Cg-Def GFGCPGNQLKCNNHCKSISCRAGY 1887
(Crassostrea gigas CDAATLWLRCTCTDCNGKK
defensin, oyster
defensin, animal
defensin)
AP01154 2B9K, LCI AIKLVQSPNGNFAASFVLDGTKWI 1888
(bacteria) FKSKYYDSSKGYWVGIYEVWDRK
AP01005 2DCV, Tachystatin YVSCLFRGARCRVYSGRSCCFGYY 1889
B1 (BBS, CRRDFPGSIFGTCSRRNF
horseshoe crabs)
AP01006 2DCW, YITCLFRGARCRVYSGRSCCFGYY 1890
Tachystatin B1 CRRDFPGSIFGTCSRRNF
(BBS, horseshoe
crabs)
AP00275 2ERI, Circulin B CGESCVFIPCISTLLGCSCKNKVCY 1891
(CirB, plant RNGVIP
cyclotides, XXC,
ZZHp)
AP00707 2f3a, LLAA (LL- RLFDKIRQVIRKF 1892
37-derived aurein
1.2 analog, retro-
FK13, synthetic)
AP00708 2fbs, FK-13 (FK13, FKRIVQRIKDFLR 1893
NMR-discovered
LL-37 core peptide,
XXA, ZZHs,
synthetic)
AP00088 2G9L, Gaegurin-4 GILDTLKQFAKGVGKDLVKGAAQ 1894
(Gaegurin 4, frog) GVLSTVSCKLAKTC
AP01011 2G9P, Latarcin 2a GLFGKLIKKFGRKAISYAVKKARG 1895
(Ltc2a, BBM, KH
spider)
AP00612 2GDL, Fowlicidin- LVQRGRFGRFLRKIRRFRPKVTITI 1896
2 (chCATH-2, bird QGSARFG
cathelicidin,
chicken
cathelicidin, BBL)
AP00402 2GL1, VrD2 KTCENLANTYRGPCFTTGSCDDHC 1897
(Vigna radiata KNKEHLRSGRCRDDFRCWCTRNC
defensin 2, plant
defensin, mung
bean)
AP00285 2GW9, Cryptdin-4 GLLCYCRKGHCKRGERVRGTCGIR 1898
(Crp4, animal FLYCCPRR
defensin, alpha,
mouse)
AP00613 2hfr, Fowlicidin-3 RVKRFWPLVPVAINTVAAGINLYK 1899
(chCATH-3, bird AIRRK
cathelicidin,
chicken
cathelicidin)
AP01007 2JMY, CM15 KWKLFKKIGAVLKVL 1900
(Synthetic)
AP00728 2jni, Arenicin-2 RWCVYAYVRIRGVLVRYRRCW 1901
(marine polychaeta,
BBBm)
AP00473 2jos, Piscidin 1 FFHHIFRGIVHVGKTIHRLVTG 1902
(fish)
AP01151 2JPJ, Lactococcin GTWDDIGQGIGRVAYWVGKALGN 1903
G-a (chain a, class LSDVNQASRINRKKKH
IIb bacteriocin,
bacteria. For chain
b, see info)
AP00757 2jpy, Phylloseptin- FLSLIPHAINAVSTLVHHF 1904
H2 (PLS-H2,
Phylloseptin-2, PS-
2) (XXA, frog)
AP00546 2jq0, Phylloseptin- FLSLIPHAINAVSAIAKHN 1905
1 (Phylloseptin-H1,
PLS-H1, PS-1,
XXA, frog)
AP00758 2jq1, Phylloseptin- FLSLIPHAINAVSALANHG 1906
3 (Phylloseptin-H3,
PLS-H3, PS-3)
(XXA, frog)
AP00727 2jsb, Arenicin-1 RWCVYAYVRVRGVLVRYRRCW 1907
(marine polychaeta,
BBBm)
AP00592 2k10, Ranatuerin- GILSSFKGVAKGVAKDLAGKLLET 1908
2CSa (frog) LKCKITGC
AP00485 2K38, Cupiennin GFGALFKFLAKKVAKTVAKQAAK 1909
1a (spider) QGAKYVVNKQME
AP00310 2K6O, Human LL- LLGDFFRKSKEKIGKEFKRIVQRIK 1910
37 (LL37, human DFLRNLVPRTES
cathelicidin;
released by
proteinase 3 from
its precursor in
neutrophils; FALL-
39; BBB, BBM,
BBP, BBW, BBD,
BBL, ZZHh)
AP00199 2LEU, Leucocin A KYYGNGVHCTKSGCSVNWGEAFS 1911
(LeuA, class IIa AGVHRLANGGNGFW
bacteriocin,
bacteria)
AP00144 2MAG, Magainin 2 GIGKFLHSAKKFGKAFVGEIMNS 1912
(frog)
AP00146 2MLT, Melittin GIGAVLKVLTTGLPALISWIKRKRQQ 1913
(insect, ZZHa)
AP01010 2PCO, Latarcin 1 SMWSGMWRRKLKKLRNALKKKL 1914
(Ltc1, BBM, KGEK
spider)
AP00176 2PM1, human ACYCRIPACIAGERRYGTCIYQGRL 1915
alpha Defensin WAFCC
HNP-1 (human
neutrophil peptide-
1, HNP1, human
defensin, ZZHh)
AP01158 2RLG, RP-1 ALYKKFKKKLLKSLKRL 1916
(synthetic)
AP00102 8TFV, Thanatin GSKKPVPIIYCNRRTGKCQRM 1917
(insect)
AP00995 A58718, Carnocin GSEIQPR 1918
UI49 (bacteria)
AP01002 AAC18827, KSWSLCTPGCARTGSFNSYCC 1919
Mutacin III
(mutacin 1140,
bacteria)
AP00987 ABI74601, Arasin SRWPSPGRPRPFPGRPKPIFRPRPCN 1920
1 (Crustacea) CYAPPCPCDRW
AP01000 CAA63706, GSGVIPTISHECHMNSFQFVFTCCS 1921
variacin
(lantibiotic, class I
bacteriocin,
bacteria)
AP00361 O15946, Lebocin 4 DLRFWNPREKLPLPTLPPFNPKPIYI 1922
(insect, silk moth) DMGNRY
AP00343 O16825, Andropin VFIDILDKMENAIHKAAQAGIGIAK 1923
(insect, fruit fly) PIEKMILPK
AP00417 O17513, SIGTAVKKAVPIAKKVGKVAIPIAK 1924
Ceratotoxin D AVLSVVGQLVG
(insect, fly)
AP00435 O18494, Styelin C GWFGKAFRSVSNFYKKHKTYIHA 1925
(sea squirt, GLSAATLL
tunicate, XXA)
AP00330 O18495, Styelin D GWLRKAAKSVGKFYYKHKYYIKA 1926
(Sea squirt, AWQIGKHAL
tunicate, XXA)
AP00331 O18495, Styelin E GWLRKAAKSVGKFYYKHKYYIKA 1927
(Sea squirt, AWKIGRHAL
tunicate, XXA)
AP01001 O54329, Mutacin II NRWWQGVVPTVSYECRMNSWQH 1928
(lantibiotic, VFTCC
mutacin H-29B, J-
T8, class I
bacteriocin,
bacteria)
AP00342 O81338, AKCIKNGKGCREDQGPPFCCSGFC 1929
Antimicrobial YRQVGWARGYCKNR
peptide 1 (plant)
AP00373 O96059, Moricin 2 AKIPIKAIKTVGKAVGKGLRAINIA 1930
(insect) STANDVFNFLKPKKRKH
AP00449 P01190, SYSMEHFRWGKPV 1931
Melanotropin alpha
(Alpha-MSH)
AP00187 P01376, VVCACRRALCLPRERRAGFCRIRG 1932
CORTICOSTATIN RIHPLCCRR
III (MCP-1, rabbit
neutrophil peptide
1, NP-1) (animal
defensin, alpha-
defensin, rabbit)
AP00188 P01377, VVCACRRALCLPLERRAGFCRIRG 1933
CORTICOSTATIN RIHPLCCRR
IV (MCP-2, rabbit
neutrophil defensin
2, NP-2, animal
defensin, rabbit)
AP00049 P01505, Bombinin GIGALSAKGALKGLAKGLAEHFAN 1934
(toad)
AP00139 P01507, Cecropin KWKLFKKIEKVGQNIRDGIIKAGP 1935
A (insect, ZZHa) AVAVVGQATQIAK
AP00128 P01509, Cecropin KWKIFKKIEKVGRNIRNGIIKAGPA 1936
B (insect, silk VAVLGEAKAL
moth)
AP00131 P01511, Cecropin WNPFKELERAGQRVRDAIISAGPA 1937
D (insect, moth) VATVAQATALAK
AP00136 P01518, Crabrolin FLPLILRKIVTAL 1938
(insect, XXA)
AP00183 P04142, Cecropin RWKIFKKIEKMGRNIRDGIVKAGP 1939
B (insect) AIEVLGSAKAI
AP00448 P04205, INLKAIAALAKKLL 1940
Mastoparan M
(MP-M, insect,
XXA)
AP00234 P06833, SDEKASPDKHHRFSLSRYAKLANR 1941
Seminalplasmin LANPKLLETFLSKWIGDRGNRSV
(SPLN, calcium
transporter
inhibitor, caltrin,
cow)
AP00314 P07466, Rabbit VFCTCRGFLCGSGERASGSCTINGV 1942
neutrophil peptide RHTLCCRR
5 (NP-5, animal
defensin, alpha-
defensin)
AP00189 P07467, Rabbit VSCTCRRFSCGFGERASGSCTVNG 1943
neutrophil peptide VRHTLCCRR
4 (NP-4)
AP00186 P07468, GRCVCRKQLLCSYRERRIGDCKIR 1944
CORTICOSTATIN GVRFPFCCPR
II (Rabbit
neutrophil peptide
3b (NP-3b, rabbit)
AP00185 P07469, ICACRRRFCPNSERFSGYCRVNGA 1945
CORTICOSTATIN RYVRCCSRR
I (rabbit)
AP00217 P07469, Rabbit GICACRRRFCPNSERFSGYCRVNG 1946
neutrophil defensin ARYVRCCSRR
3a (NP-3a, animal
defensin, alpha-
defensin)
AP00067 P07493, SKITDILAKLGKVLAHV 1947
Bombolitin II
(insect, bee)
AP00068 P07494, IKIMDILAKLGKVLAHV 1948
Bombolitin III
(insect, bee)
AP00069 P07495, INIKDILAKLVKVLGHV 1949
Bombolitin IV
(insect, bee)
AP00070 P07496, INVLGILGLLGKALSHL 1950
Bombolitin V
(insect, bee)
AP00236 P07504, Pyrularia KSCCRNTWARNCYNVCRLPGTISR 1951
thionin (Pp-TH, EICAKKCDCKIISGTTCPSDYPK
plant)
AP00230 P08375, Sarcotoxin GWLKKIGKKIERVGQHTRDATIQG 1952
IA (insect, flesh LGIAQQAANVAATAR
AP00231 P08376, Sarcotoxin GWLKKIGKKIERVGQHTRDATIQV 1953
IB (insect, flesh IGVAQQAANVAATAR
AP00232 P08377, Sarcotoxin GWLRKIGKKIERVGQHTRDATIQV 1954
IC (insect, flesh LGIAQQAANVAATAR
AP00066 P10521, IKITTMLAKLGKVLAHV 1955
Bombolitin I
(insect, bee)
AP00206 P10946, Lantibiotic WKSESLCTPGCVTGALQTCFLQTL 1956
subtilin (class I TCNCKISK
bacteriocin,
bacteria)
AP00312 P11477, Cryptdin-2 LRDLVCYCRARGCKGRERMNGTC 1957
(Crp2, animal RKGHLLYMLCCR
defensin, alpha,
mouse)
AP00205 P13068, Nisin A ITSISLCTPGCKTGALMGCNMKTA 1958
(lantibiotic, class I TCHCSIHVSK
bacteriocin,
bacteria)
AP00215 P14214, RWCFRVCYRGICYRKCR 1959
Tachyplesin II
(crabs, Crustacea)
AP00212 P14216, RRWCFRVCYKGFCYRKCR 1960
Polyphemusin II
(crabs, Crustacea,
XXA, ZZHa.
Derivatives: T22)
AP00134 P14661, Cecropin SWLSKTAKKLENSAKKRISEGIAIA 1961
P1 (pig) IQGGPR
AP00011 P14662, WNPFKELERAGQRVRDAVISAAPA 1962
Bactericidin B2 VATVGQAAAIARG
(insect)
AP00032 P14663, WNPFKELERAGQRVRDAIISAGPA 1963
Bactericidin B-3 VATVGQAAAIARG
(insect)
AP00033 P14664, WNPFKELERAGQRVRDAIISAAPA 1964
Bactericidin B-4 VATVGQAAAIARG
(insect)
AP00034 P14665, WNPFKELERAGQRVRDAVISAAA 1965
Bactericidin B-5P VATVGQAAAIARG
(insect)
AP00125 P14666, Cecropin RWKIFKKIEKVGQNIRDGIVKAGP 1966
(insect, silk moth) AVAVVGQAATI
AP00002 P15450, YVPLPNVPQPGRRPFPTFPGQGPFN 1967
ABAECIN (insect, PKIKWPQGY
honeybee)
AP00505 P15516, human DSHAKRHHGYKRKFHEKHHSHRGY 1968
Histatin 5 (ZZHs;
derivatives Dh-5)
AP00520 P15516, human DSHAKRHHGYKRKFHEKHHSHRG 1969
Histatin 3 YRSNYLYDN
AP00523 P15516, human KFHEKHHSHRGY 1970
Histatin 8
AP00226 P17722, Royalisin VTCDLLSFKGQVNDSACAANCLSL 1971
(insect, honeybee) GKAGGHCEKVGCICRKTSFKDLW
DKRF
AP00213 P18252, KWCFRVCYRGICYRKCR 1972
Tachyplesin III
(horseshoe crabs,
Crustacea)
AP00233 P18312, Sarcotoxin GWIRDFGKRIERVGQHTRDATIQTI 1973
ID (insect, flesh AVAQQAANVAATLKG
AP00207 P19578, Lantibiotic TAGPAIRASVKQCQKTLKATRLFT 1974
PEP5 (class I VSCKGKNGCK
bacteriocin,
bacteria)
AP00009 P19660, RFRPPIRRPPIRPPFYPPFRPPIRPPIF 1975
BACTENECIN 5 PPIRPPFRPPLGPFP
(bac5, cow
cathelicidin)
AP00010 P19661, RRIRPRPPRLPRPRPRPLPFPRPGPR 1976
BACTENECIN 7 PIPRPLPFPRPGPRPIPRPLPFPRPGP
(bac7, cow RPIPRPL
cathelicidin)
AP00200 P21564, LKLKSIVSWAKKVL 1977
Mastoparan B
(MP-B, insect,
XXA)
AP00005 P21663, Andropin VFIDILDKVENAIHNAAQVGIGFAK 1978
(insect, fly) PFEKLINPK
AP00008 P22226, Cyclic RLCRIVVIRVCR 1979
dodecapeptide
(cow cathelicidin)
AP01205 P23826, Lactocin S STPVLASVAVSMELLPTASVLYSD 1980
(XXD3, bacteria) VAGCFKYSAKHHC
AP00239 P24335, XPF (the GWASKIGQTLGKIAKVGLKELIQPK 1981
xenopsin precursor
fragment, African
clawed frog)
AP00235 P25068, Bovine NPVSCVRNKGICVPIRCPGSMKQIG 1982
tracheal TCVGRAVKCCRKK
antimicrobial
peptide (TAP, cow)
AP00418 P25230, CAP18 GLRKRLRKFRNKIKEKLKKIGQKIQ 1983
(rabbit cathelicidin, GFVPKLAPRTDY
BBL)
AP00203 P25403, Mj-AMP1 QCIGNGGRCNENVGPPYCCSGFCL 1984
(MjAMP1, plant RQPGQGYGYCKNR
defensin)
AP00202 P25404, Mj-AMP2 CIGNGGRCNENVGPPYCCSGFCLR 1985
(MjAMP2, plant QPNQGYGVCRNR
defensin)
AP00138 P28310, Cryptdin-3 LRDLVCYCRKRGCKRRERMNGTC 1986
(Crp3, animal RKGHLMYTLCCR
defensin, alpha,
mouse)
AP00184 P28794, MBP-1 RSGRGECRRQCLRRHEGQPWETQ 1987
(plant) ECMRRCRRRG
AP00050 P29002, Bombinin- GIGASILSAGKSALKGLAKGLAEHF 1988
like peptide 1 AN
(BLP-1, toad)
AP00051 P29003, Bombinin- GIGSAILSAGKSALKGLAKGLAEHF 1989
like peptide 2 AN
(BLP-2, toad)
AP00052 P29004, Bombinin- GIGAAILSAGKSALKGLAKGLAEHF 1990
like peptide 3
(BLP-3, XXA,
toad)
AP00053 P29005, Bombinin- GIGAAILSAGKSIIKGLANGLAEHF 1991
like peptide 4
(BLP-4, toad)
AP00634 P29430, Pediocin KYYGNGVTCGKHSCSVDWGKATT 1992
PA-1/AcH CIINNGAMAWATGGHQGNHKC
(PedPA1, class IIA
bacteriocin, bacteria)
AP00204 P29559, Nisin Z ITSISLCTPGCKTGALMGCNMKTA 1993
(lantibiotic, class I TCNCSIHVSK
bacteriocin,
bacteria)
AP00130 P29561, Cecropin GWLKKLGKRIERIGQHTRDATIQG 1994
C (insect, fly) LGIAQQAANVAATAR
AP00001 P31107, GLWSKIKEVGKEAAKAAAKAAGK 1995
ADENOREGULIN AALGAVSEAV
(Dermaseptin B2,
Dermaseptin-B2,
DRS-B2, DRS B2,
frog)
AP00228 P31529, Sapecin B LTCEIDRSLCLLHCRLKGYLRAYCS 1996
(insect, flesh fly) QQKVCRCVQ
AP00229 P31530, Sapecin C ATCDLLSGIGVQHSACALHCVFRG 1997
(insect, flesh fly) NRGGYCTGKGICVCRN
AP00218 P32195, Protegrin RGGRLCYCRRRFCICV 1998
2 (PG-2, pig
cathelicidin)
AP00219 P32196, Protegrin RGGGLCYCRRRFCVCVGR 1999
3 (PG-3, pig
cathelicidin)
AP00073 P32412, Brevinin- FLPLLAGLAANFLPKIFCKITRKC 2000
1E (frog)
AP00080 P32414, GIFSKLGRKKIKNLLISGLKNVGKE 2001
Esculentin-1 (frog) VGMDVVRTGIDIAGCKIKGEC
AP00074 P32423, Brevinin-1 FLPVLAGIAAKVVPALFCKITKKC 2002
(frog)
AP00075 P32424, Brevinin-2 GLLDSLKGFAATAGKGVLQSLLST 2003
(frog) ASCKLAKTC
AP00175 P34084, Macaque DSHEERHHGRHGHHKYGRKFHEK 2004
histatin (M-Histatin HHSHRGYRSNYLYDN
1, primate,
monkey)
AP00006 P35581, Apidaecin GNNRPVYIPQPRPPHPRI 2005
IA (insect,
honeybee)
AP00007 P35581, Apidaecin GNNRPVYIPQPRPPHPRL 2006
IB (insect,
honeybee)
AP00414 P36190, SIGSALKKALPVAKKIGKIALPIAK 2007
Ceratotoxin A AALP
(insect, fly)
AP00415 P36191, SIGSAFKKALPVAKKIGKAALPIAK 2008
Ceratotoxin B AALP
(insect, fly)
AP00172 P36193, Drosocin GKPRPYSPRPTSHPRPIRV 2009
(insect)
AP00170 P37362, VDKGSYLPRPTPPRPIYNRN 2010
Pyrrhocoricin
(insect)
AP00635 P38577, KYYGNGVHCTKSGCSVNWGEAAS 2011
Mesentericin Y105 AGIHRLANGGNGFW
(MesY105, class
IIA bacteriocin,
bacteria)
AP00636 P38579, AISYGNGVYCNKEKCWVNKAENK 2012
Carnobacteriocin QAITGIVIGGWASSLAGMGH
BM1 (CnbBM1,
PiscV1b, class IIA
bacteriocin,
bacteria)
AP00209 P39080, Peptide GVLSNVIGYLKKLGTGALNAVLKQ 2013
PGQ (frog)
AP00513 P39084, Ranalexin FLGGLIKIVPAMICAVTKKC 2014
(frog)
AP00071 P40835, Brevinin- FLPAIFRMAAKVVPTIICSITKKC 2015
1EA (frog)
AP00072 P40836, Brevinin- VIPFVASVAAEMQHVYCAASRKC 2016
1EB (frog)
AP00076 P40837, Brevinin- GILDTLKNLAISAAKGAAQGLVNK 2017
2EA (frog) ASCKLSGQC
AP00077 P40838, Brevinin- GILDTLKNLAKTAGKGALQGLVK 2018
2EB (frog) MASCKLSGQC
AP00078 P40839, Brevinin- GILLDKLKNFAKTAGKGVLQSLLN 2019
2EC (frog) TASCKLSGQC
AP00079 P40840, Brevinin- GILDSLKNLAKNAGQILLNKASCK 2020
2ED (frog) LSGQC
AP00081 P40843, GIFSKLAGKKIKNLLISGLKNVGKE 2021
Esculentin-1A VGMDVVRTGIDIAGCKIKGEC
(frog)
AP00082 P40844, GIFSKLAGKKLKNLLISGLKNVGK 2022
Esculentin-1B EVGMDVVRTGIDIAGCKIKGEC
(frog)
AP00083 P40845, GILSLVKGVAKLAGKGLAKEGGKF 2023
Esculentin-2A GLELIACKIAKQC
(frog)
AP00084 P40846, GIFSLVKGAAKLAGKGLAKEGGKF 2024
Esculentin-2B GLELIACKIAKQC
(ES2B_RANES,
frog)
AP00299 P46156, Chicken GRKSDCFRKSGFCAFLKCPSLTLIS 2025
gallinacin 1 (Gal 1, GKCSRFYLCCKRIW
avian beta-
defensin, bird)
AP00300 P46157, Gallinacin GRKSDCFRKNGFCAFLKCPYLTLIS 2026
1 alpha (avian beta- GKCSRFHLCCKRIW
defensin, Bird),
AP00298 P46158, Chicken LFCKGGSCHFGGCPSHLIKVGSCFG 2027
gallinacin 2 (Gal 2, FRSCCKWPWNA
avian beta-
defensin, bird)
AP00037 P46160, Beta- VRNHVTCRINRGFCVPIRCPGRTRQ 2028
defensin 2 (cow) IGTCFGPRIKCCRSW
AP00038 P46161, Beta- QGVRNHVTCRINRGFCVPIRCPGR 2029
defensin 3 (cow) TRQIGTCFGPRIKCCRSW
AP00039 P46162, Beta- QRVRNPQSCRWNMGVCIPFLCRV 2030
defensin 4 (cow) GMRQIGTCFGPRVPCCRR
AP00040 P46163, Beta- QVVRNPQSCRWNMGVCIPISCPGN 2031
defensin 5 (cow) MRQIGTCFGPRVPCCRRW
AP00041 P46164, Beta- QGVRNHVTCRIYGGFCVPIRCPGR 2032
defensin 6 (cow) TRQIGTCFGRPVKCCRRW
AP00042 P46165, Beta- QGVRNFVTCRINRGFCVPIRCPGHR 2033
defensin 7 (cow) RQIGTCLGPRIKCCR
AP00043 P46166, Beta- VRNFVTCRINRGFCVPIRCPGHRRQ 2034
defensin 8 (cow) IGTCLGPQIKCCR
AP00044 P46167, Beta- QGVRNFVTCRINRGFCVPIRCPGHR 2035
defensin 9 (cow) RQIGTCLAPQIKCCR
AP00045 P46168, Beta- QGVRSYLSCWGNRGICLLNRCPGR 2036
defensin 10 (cow) MRQIGTCLAPRVKCCR
AP00046 P46169, Beta- GPLSCRRNGGVCIPIRCPGPMRQIG 2037
defensin 11 (cow) TCFGRPVKCCRSW
AP00048 P46171, Bovine SGISGPLSCGRNGGVCIPIRCPVPM 2038
beta-defensin 13 RQIGTCFGRPVKCCRSW
(cow)
AP00350 P48821, Enbocin PWNIFKEIERAVARTRDAVISAGPA 2039
(insect, moth) VRTVAAATSVAS
AP00173 P49112, GNCP-2 RCICTTRTCRFPYRRLGTCLFQNRV 2040
(Guinea pig YTFCC
neutrophil cationic
peptide 2)
AP00369 P49930, PMAP-23 RIIDLLWRVRRPQKPKFVTVWVR 2041
(PMAP23, pig
cathelicidin)
AP00370 P49931, PMAP-36 VGRFRRLRKKTRKRLKKIGKVLK 2042
(PMAP36, pig WIPPIVGSIPLGCG
cathelicidin)
AP00371 P49932, PMAP-37 GLLSRLRDFLSDRGRRLGEKIERIG 2043
(PMAP37, pig QKIKDLSEFFQS
cathelicidin)
AP00220 P49933, Protegrin RGGRLCYCRGWICFCVGR 2044
4 (PG-4, pig
cathelicidin)
AP00221 P49934, Protegrin RGGRLCYCRPRFCVCVGR 2045
5 (PG-5, pig
cathelicidin)
AP00346 P50720, Hyphancin RWKIFKKIERVGQNVRDGIIKAGP 2046
IIID (Fall AIQVLGTAKAL
webworm, insect)
AP00347 P50721, Hyphancin RWKFFKKIERVGQNVRDGLIKAGP 2047
IIIE (Fall AIQVLGAAKAL
webworm, insect)
AP00348 P50722, Hyphancin RWKVFKKIEKVGRNIRDGVIKAGP 2048
IIIF (Fall AIAVVGQAKAL
webworm, insect)
AP00349 P50723, Hyphancin RWKVFKKIEKVGRHIRDGVIKAGP 2049
IIIG (Fall AITVVGQATAL
webworm, insect)
AP00281 P51473, mCRAMP GLLRKGGEKIGEKLKKIGQKIKNFF 2050
(mouse QKLVPQPEQ
cathelicidin;
derivatives:
CRAMP 18)
AP00366 P54228, BMAP-27 GRFKRFRKKFKKLFKKLSPVIPLLH 2051
(BMAP27, cow LG
cathelicidin, ZZHs,
derivatives BMAP-
18 and BMAP-15)
AP00367 P54229, BMAP-28 GGLRSLGRKILRAWKKYGPIIVPIIR 2052
(BMAP28, cow IG
cathelicidin)
AP00450 P54230, Cyclic RICRIIFLRVCR 2053
dodecapeptide
(sheep cathelicidin)
AP00359 P54684, Lebocin DLRFLYPRGKLPVPTPPPFNPKPIYI 2054
½ (insect, silk DMGNRY
moth)
AP00360 P55796, Lebocin 3 DLRFLYPRGKLPVPTLPPFNPKPIYI 2055
(insect, silk moth) DMGNRY
AP00307 P55897, Buforin I AGRGKQGGKVRAKAKTRSSRAGL 2056
(toad) QFPVGRVHRLLRKGNY
AP00308 P55897, Buforin II TRSSRAGLQFPVGRVHRLLRK 2057
(toad)
AP00240 P56226, Caerin 1.1 GLLSVLGSVAKHVLPHVVPVIAEHL 2058
(frog, ZZHa)
AP00241 P56227, Caerin 1.2 GLLGVLGSVAKHVLPHVVPVIAEHL 2059
(frog)
AP00242 P56228, Caerin 1.3 GLLSVLGSVAQHVLPHVVPVIAEHL 2060
(frog)
AP00243 P56229, Caerin 1.4 GLLSSLSSVAKHVLPHVVPVIAEHL 2061
(frog)
AP00244 P56230, Caerin 1.5 GLLSVLGSVVKHVIPHVVPVIAEHL 2062
(frog)
AP00245 P56231, Caerin 1.6 GLFSVLGAVAKHVLPHVVPVIAEK 2063
(frog)
AP00246 P56232, Caerin 1.7 GLFKVLGSVAKHLLPHVAPVIAEK 2064
(frog)
AP00249 P56233, Caerin 2.1 GLVSSIGRALGGLLADVVKSKGQPA 2065
(frog)
AP00250 P56234, Caerin 2.2 GLVSSIGRALGGLLADVVKSKEQPA 2066
(frog)
AP00251 P56236, Caerin 2.4 GLVSSIGKALGGLLADVVKTKEQPA 2067
(frog)
AP00252 P56236, Caerin 2.5 GLVSSIGRALGGLLADVVKSKEQPA 2068
(frog)
AP00253 P56238, Caerin 3.1 GLWQKIKDKASELVSGIVEGVK 2069
(frog)
AP00254 P56238, Caerin 3.2 GLWEKIKEKASELVSGIVEGVK 2070
(frog)
AP00255 P56240, Caerin 3.3 GLWEKIKEKANELVSGIVEGVK 2071
(frog)
AP00256 P56241, Caerin 3.4 GLWEKIREKANELVSGIVEGVK 2072
(frog)
AP00257 P56242, Caerin 4.1 GLWQKIKSAAGDLASGIVEGIKS 2073
(frog)
AP00258 P56243, Caerin 4.2 GLWQKIKSAAGDLASGIVEGIKS 2074
(frog)
AP00259 P56244, Caerin 4.3 GLWQKIKNAAGDLASGIVEGIKS 2075
(frog)
AP00434 P56249, Frenatin 3 GLMSVLGHAVGNVLGGLFKS 2076
(frog)
AP00272 P56386, Murine DQYKCLQHGGFCLRSSCPSNTKLQ 2077
beta-defensin 1 GTCKPDKPNCCKS
(mBD-1, mouse)
AP00368 P56425, BMAP-34 GLFRRLRDSIRRGQQKILEKARRIG 2078
(BMAP34, cow ERIKDIFRG
cathelicidin)
AP00273 P56685, Buthinin SIVPIRCRSNRDCRRFCGFRGGRCT 2079
(Sahara scorpion) YARQCLCGY
AP00282 P56872, SIPCGESCVFIPCTVTALLGCSCKSK 2080
Cyclopsychotride VCYKN
A (CPT, plant
cyclotides, XXC)
AP00094 P56917, Temporin FLPLIGRVLSGIL 2081
A (XXA, frog)
AP00096 P56918, Temporin LLPILGNLLNGLL 2082
C (XXA, frog)
AP00097 P56920, Temporin VLPIIGNLLNSLL 2083
E (XXA, frog)
AP00098 P56921, Temporin FLPLIGKVLSGIL 2084
F (XXA, frog)
AP00100 P56923, Temporin LLPNLLKSLL 2085
K (XXA, frog)
AP00295 P56928, eNAP-2 EVERKHPLGGSRPGRCPTVPPGTF 2086
(horse) GHCACLCTGDASEPKGQKCCSN
AP00101 P57104, Temporin FVQWFSKFLGRIL 2087
L (XXA, frog)
AP00095 P79874, Temporin LLPIVGNLLKSLL 2088
B (XXA, frog)
AP00099 P79875, Temporin FFPVIGRILNGIL 2089
G (XXA, frog)
AP00413 P80032, SLQGGAPNFPQPSQQNGGWQVSP 2090
Coleoptericin DLGRDDKGNTRGQIEIQNKGKDH
(insect) DFNAGWGKVIRGPNKAKPTWHVG
GTYRR
AP00396 P80054, PR-39 RRRPRPPYLPRPRPPPFFPPRLPPRIP 2091
(PR39, pig PGFPPRFPPRFP
cathelicidin)
AP00182 P80154, Insect GFGCPLDQMQCHRHCQTITGRSGG 2092
defensin YCSGPLKLTCTCYR
AP00444 P80223, GICACRRRFCLNFEQFSGYCRVNG 2093
Corticostatin VI ARYVRCCSRR
(CS-VI) (animal
defensin, rabbit)
AP00208 P80230, Peptide RADTQTYQPYNKDWIKEKIYVLLR 2094
3910 (pig) RQAQQAGK
AP00157 P80277, ALWKTMLKKLGTMALHAGKAAL 2095
Dermaseptin-S1 GAAADTISQGTQ
(Dermaseptin S1,
DRS S1, DRS-S1,
frog)
AP00158 P80278, ALWFTMLKKLGTMALHAGKAAL 2096
Dermaseptin-S2 GAAANTISQGTQ
(Dermaseptin S2,
DRS S2, DRS-S2,
frog)
AP00159 P80279, ALWKNMLKGIGKLAGKAALGAV 2097
Dermaseptin-S3 KKLVGAES
(Dermaseptin S3,
DRS S3, DRS-S3,
frog)
AP00160 P80280, ALWMTLLKKVLKAAAKALNAVL 2098
Dermaseptin-S4 VGANA
(Dermaseptin S4,
DRS S4, DRS-S4,
frog)
AP00161 P80281, GLWSKIKTAGKSVAKAAAKAAVK 2099
Dermaseptin-S5 AVTNAV
(Dermaseptin S5,
DRS S5, DRS-S5,
frog)
AP00293 P80282, AMWKDVLKKIGTVALHAGKAAL 2100
Dermaseptin-B1 GAVADTISQ
(DRS-B1, DRS B1,
frog)
AP00264 P80389, Chicken GRKSDCFRKSGFCAFLKCPSLTLIS 2101
Heterophil Peptide GKCSRFYLCCKRIR
1 (CHP1, bird,
animal)
AP00265 P80390, Chicken GRKSDCFRKNGFCAFLKCPYLTLIS 2102
Heterophil Peptide GLCSFHLC
2 (CHP2, bird,
animal)
AP00266 P80391, Turkey GKREKCLRRNGFCAFLKCPTLSVIS 2103
Heterophil Peptide GTCSRFQVCC
1 (THP1, turkey)
AP00267 P80392, Turkey LFCKRGTCHFGRCPSHLIKVGSCFG 2104
Heterophil Peptide FRSCCKWPWDA
2 (THP2, bird,
anaimal)
AP00269 P80393, Turkey LSCKRGTCHFGRCPSHLIKGSCSGG 2105
Heterophil Peptide
3 (THP3, bird,
animal)
AP00085 P80395, Gaegurin- SLFSLIKAGAKFLGKNLLKQGACY 2106
1 (Gaegurin 1, AACKASKQC
frog)
AP00086 P80396, Gaegurin- GIMSIVKDVAKNAAKEAAKGALST 2107
2 (Gaegurin 2, LSCKLAKTC
frog)
AP00087 P80397, Gaegurin- GIMSIVKDVAKTAAKEAAKGALST 2108
3 (Gaegurin 3, LSCKLAKTC
frog)
AP00089 P80399, Gaegurin- FLGALFKVASKVLPSVFCAITKKC 2109
5 (Gaegurin 5,
frog)
AP00090 P80400, Gaegurin- FLPLLAGLAANFLPTIICKISYKC 2110
6 (Gaegurin 6,
frog)
AP00362 P80408, VDKPDYRPRPRPPNM 2111
Metalnikowin I
(insect)
AP00363 P80409, VDKPDYRPRPWPRPN 2112
Metalnikowin IIA
(insect)
AP00364 P80410, VDKPDYRPRPWPRNMI 2113
Metalnikowin IIB
(insect)
AP00365 P80411, VDKPDYRPRPWPRPNM 2114
Metalnikowin III
(insect)
AP00632 P80569, Piscicolin KYYGNGVSCNKNGCTVDWSKAIG 2115
126/Piscicocin IIGNNAAANLTTGGAAGWNKG
Via (PiscV1a,
Pisc126, class IIA
bacteriocin,
bacteria)
AP01003 P80666, Mutacin FKSWSFCTPGCAKTGSFNSYCC 2116
B-Ny266 (bacteria)
AP00276 P80710, Clavanin VFQFLGKIIHHVGNFVHGFSHVF 2117
A (urochordates,
sea squirts, and sea
pork, tunicate)
AP00277 P80711, Clavanin VFQFLGRIIHHVGNFVHGFSHVF 2118
B (Sea squirt,
tunicate)
AP00278 P80712, Clavanin VFHLLGKIIHHVGNFVYGFSHVF 2119
C (Sea squirt,
tunicate)
AP00279 P80713, Clavanin AFKLLGRIIHHVGNFVYGFSHVF 2120
D (Sea squirt,
tunicate)
AP00280 P80713, Clavanin LFKLLGKIIHHVGNFVHGFSHVF 2121
D (Sea squirt,
tunicate)
AP00294 P80930, eNAP-1 DVQCGEGHFCHDQTCCRASQGGA 2122
(horse) CCPYSQGVCCADQRHCCPVGF
AP00400 P80952, Skin YPPKPESPGEDASPEEMNKYLTAL 2123
peptide tyrosine- RHYINLVTRQRY
tyrosine (skin-
PYY, SPYY, frog)
AP00091 P80954, Rugosin A GLLNTFKDWAISIAKGAGKGVLTT 2124
(frog) LSCKLDKSC
AP00092 P80955, Rugosin B SLFSLIKAGAKFLGKNLLKQGAQY 2125
(frog) AACKVSKEC
AP00093 P80956, Rugosin C GILDSFKQFAKGVGKDLIKGAAQG 2126
(frog) VLSTMSCKLAKTC
AP00392 P81056, Penaeidin- YRGGYTGPIPRPPPIGRPPLRLVVC 2127
1 (shrimp, ACYRLSVSDARNCCIKFGSCCHLVK
Crustacea)
AP00393 P81057, Penaeidin- YRGGYTGPIPRPPPIGRPPFRPVCN 2128
2a (shrimp, ACYRLSVSDARNCCIKFGSCCHLVK
Crustacea)
AP00394 P81058, Penaeidin- QVYKGGYTRPIPRPPPFVRPLPGGP 2129
3a (shrimp, IGPYNGCPVSCRGISFSQARSCCSR
Crustacea) LGRCCHVGKGYS
AP00247 P81251, Caerin 1.8 GLFKVLGSVAKHLLPHVVPVIAEK 2130
(frog)
AP00248 P81252, Caerin 1.9 GLFGVLGSIAKHVLPHVVPVIAEK 2131
(frog, ZZHa)
AP00126 P81417, Cecropin GGLKKLGKKLEGVGKRVFKASEK 2132
A (insect, ALPVAVGIKALG
mosquito)
AP00169 P81437, Formaecin GRPNPVNTKPTPYPRL 2133
2 (insect, ants)
AP00168 P81438, Formaecin GRPNPVNNKPTPHPRL 2134
1 (insect, ants)
AP00296 P81456, Fabatin-1 LLGRCKVKSNRFHGPCLTDTHCST 2135
(plant defensin) VCRGEGYKGGDCHGLRRRCMCLC
AP00297 P81457, Fabatin-2 LLGRCKVKSNRFNGPCLTDTHCST 2136
(plant defensin) VCRGEGYKGGDCHGLRRRCMCLC
AP01215 P81463, European FVPYNPPRPYQSKPFPSFPGHGPFN 2137
bumblebee abaecin PKIQWPYPLPNPGH
(insect)
AP01214 P81464, Apidaecin GNRPVYIPPPRPPHPRL 2138
(insect)
AP00440 P81465, defensin VTCFCRRRGCASRERHIGYCRFGN 2139
HANP-1 (hamster) TIYRLCCRR
AP00441 P81466, defensin CFCKRPVCDSGETQIGYCRLGNTF 2140
HANP-2 (hamster) YRLCCRQ
AP00442 P81467, defensin VTCFCRRRGCASRERLIGYCRFGN 2141
HANP-3 (hamster) TIYGLCCRR
AP00439 P81468, defensin VTCFCKRPVCDSGETQIGYCRLGN 2142
HANP-4 (hamster) TFYRLCCRQ
AP00328 P81469, Styelin A GFGKAFHSVSNFAKKHKTA 2143
(Sea squirt,
tunicate, XXA)
AP00329 P81470, Styelin B GFGPAFHSVSNFAKKHKTA 2144
(Sea squirt,
tunicate, XXA)
AP00492 P81474, Misgurin RQRVEELSKFSKKGAAARRRK 2145
(fish)
AP00165 P81485, ALWKNMLKGIGKLAGQAALGAV 2146
Dermaseptin-B3 KTLVGAE
(Dermaseptin B3,
DRS-B3, DRS B3,
frog)
AP00163 P81486, ALWKDILKNVGKAAGKAVLNTVT 2147
Dermaseptin-B4 DMVNQ
(Dermaseptin B4,
DRS-B4, DRS B4,
DRS-TR1, IRP,
frog)
AP00162 P81487, GLWNKIKEAASKAAGKAALGFVN 2148
Dermaseptin-B5 EMV
(Dermaseptin B5,
DRS-B5, DRS B5,
frog)
AP00164 P81488, ALWKTIIKGAGKMIGSLAKNLLGS 2149
Dermaseptin-B9 QAQPES
(Dermaseptin B9,
DRS-B9, DRS
DRG3, frog)
AP00167 P81565, Phylloxin GWMSKIASGIGTFLSGMQQ 2150
(phylloxin-B1,
PLX-B1, XXA,
frog)
AP00291 P81568, Defensin MFFSSKKCKTVSKTFRGPCVRNAN 2151
D5 (So-D5) (plant
defensin)
AP00290 P81569, Defensin MFFSSKKCKTVSKTFRGPCVRNA 2152
D4 (So-D4) (plant
defensin)
AP00289 P81570, Defensin GIFSSRKCKTVSKTFRGICTRNANC 2153
D3 (So-D3) (plant
defensin)
AP00288 P81572, Defensin TCESPSHKFKGPCATNRNCES 2154
D1 (So-D1) (plant
defensin)
AP00292 P81573, Defensin GIFSSRKCKTPSKTFKGYCTRDSNC 2155
D7 (So-D7) (plant DTSCRYEGYPAGD
defensin)
AP00270 P81591, Pn-AMP QQCGRQASGRLCGNRLCCSQWGY 2156
(PnAMP, plant CGSTASYCGAGCQSQCRS
defensin)
AP00412 P81592, SLQPGAPNVNNKDQPWQVSPHISR 2157
Acaloleptin A1 DDSGNTRTDINVQRHGENNDFEAG
(insect) WSKVVRGPNKAKPTWHIGGTHRW
AP00433 P81605, human SSLLEKGLDGAKKAVGGLGKLGK 2158
Dermcidin (DCD- DAVEDLESVGKGAVHDVKDVLDSV
1)
AP00332 P81612, Mytilin A GCASRCKAKCAGRRCKGWASASF 2159
(Blue mussel) RGRCYCKCFRC
AP00333 P81613, Mytilin B SCASRCKGHCRARRCGYYVSVLY 2160
(Blue mussel) RGRCYCKCLRC
AP00334 P81613, FFHHIFRGIVHVGKTIHKLVTG 2161
Moronecidin (fish)
AP00351 P81835, Citropin GLFDVIKKVASVIGGL 2162
1.1 (amphibian,
frog)
AP00352 P81840, Citropin GLFDIIKKVASVVGGL 2163
1.2 (amphibian,
frog)
AP00353 P81846, Citropin GLFDIIKKVASVIGGL 2164
1.3 (amphibian,
frog)
AP00338 P81903, Histone PDPAKTAPKKGSKKAVTKA 2165
H2B-1(HLP-1)
(fish)
AP00271 P82018, ChBac5 RFRPPIRRPPIRPPFNPPFRPPVRPPF 2166
(Goat cathelicidin) RPPFRPPFRPPIGPFP
AP00316 P82027, Uperin 2.1 GIVDFAKKVVGGIRNALGI 2167
(amphibian, toad)
AP00317 P82028, Uperin 2.2 GFVDLAKKVVGGIRNALGI 2168
(amphibian, toad)
AP00318 P82029, Uperin 2.3 GFFDLAKKVVGGIRNALGI 2169
(amphibian, toad)
AP00319 P82030, Uperin 2.4 GILDFAKTVVGGIRNALGI 2170
(amphibian, toad)
AP00320 P82031, Uperin 2.5 GIVDFAKGVLGKIKNVLGI 2171
(amphibian, toad)
AP00323 P82032, Uperin 3.1 GVLDAFRKIATVVKNVV 2172
(amphibian, toad)
AP00326 P82035, Uperin 4.1 GVGSFIHKVVSAIKNVA 2173
(amphibian, toad)
AP00321 P82039, Uperin 2.7 GIIDIAKKLVGGIRNVLGI 2174
(amphibian, toad)
AP00322 P82040, Uperin 2.8 GILDVAKTLVGKLRNVLGI 2175
(amphibian, toad)
AP00324 P82042, Uperin 3.5 GVGDLIRKAVSVIKNIV 2176
(amphibian, toad)
AP00325 P82042, Uperin 3.6 GVIDAAKKVVNVLKNLP 2177
(amphibian, toad)
AP00327 P82050, Uperin 7.1 GWFDVVKHIASAV 2178
(amphibian, frog)
AP00260 P82066, Maculatin GLFVGVLAKVAAHVVPAIAEHF 2179
1.1 (XXA, frog,
ZZHa)
AP00261 P82067, Maculatin GLFVGLAKVAAHNNPAIAEHFQA 2180
1.2 (XXA, frog)
AP00262 P82068, Maculatin GFVDFLKKVAGTIANVVT 2181
2.1 (frog)
AP00263 P82069, Maculatin GLLQTIKEKLESLESLAKGIVSGIQA 2182
3.1 (frog)
AP00345 P82104, Caerin GLLSVLGSVAKHVLPHVVPVIAEKL 2183
1.10 (frog)
AP00456 P82232, Brevinin- VNPIILGVLPKFVCLITKKC 2184
1T (frog)
AP00459 P82233, Brevinin- FITLLLRKFICSITKKC 2185
1TA (frog)
AP00457 P82234, Brevinin- GLWETIKNFGKKFTLNILHKLKCKI 2186
2TC (frog) GGGC
AP00458 P82235, Brevinin- GLWETIKNFGKKFTLNILHNLKCKI 2187
2TD (frog) GGGC
AP00397 P82238, SGFVLKGYTKTSQ 2188
Salmocidin 2A
(fish, trout)
AP00398 P82239, AGFVLKGYTKTSQ 2189
Salmocidin 2B
(fish, trout)
AP00055 P82282, Bombinin IIGPVLGMVGSALGGLLKKI 2190
H1 (frog)
AP00056 P82284, Bombinin LIGPVLGLVGSALGGLLKKI 2191
H4 (frog, XXA,
XXD)
AP00057 P82285, Bombinin IIGPVLGLVGSALGGLLKKI 2192
H5 (frog, XXD)
AP00419 P82286, Bombinin- GIGASILSAGKSALKGFAKGLAEHF 2193
like peptides 2 AN
(amphibian, toad)
AP00137 P82293, Cryptdin-1 LRDLVCYCRTRGCKRRERMNGTC 2194
(Crp1, animal RKGHLMYTLCCR
defensin, alpha,
mouse)
AP00443 P82317, defensin ACYCRIPACLAGERRYGTCFYMGR 2195
RMAD-2 (monkey) VWAFCC
AP00012 P82386, Aurein 1.1 GLFDIIKKIAESI 2196
(amphibian, frog)
AP00014 P82388, Aurein 2.1 GLLDIVKKVVGAFGSL 2197
(amphibian, frog)
AP00015 P82389, Aurein 2.2 GLFDIVKKVVGALGSL 2198
(amphibian, frog)
AP00016 P82390, Aurein 2.3 GLFDIVKKVVGAIGSL 2199
(XXA,
amphibian, frog)
AP00017 P82391, Aurein 2.4 GLFDIVKKVVGTIAGL 2200
(XXA,
amphibian, frog)
AP00018 P82392, Aurein 2.5 GLFDIVKKVVGAFGSL 2201
(XXA,
amphibian, frog)
AP00019 P82393, Aurein 2.6 GLFDIAKKVIGVIGSL 2202
(XXA,
amphibian, frog)
AP00020 P82394, Aurein 3.1 GLFDIVKKIAGHIAGSI 2203
(XXA,
amphibian, frog)
AP00021 P82395, Aurein 3.2 GLFDIVKKIAGHIASSI 2204
(XXA,
amphibian, frog)
AP00022 P82396, Aurein 3.3 GLFDIVKKIAGHIVSSI 2205
(XXA,
amphibian, frog)
AP00376 P82414, Ponericin GWKDWAKKAGGWLKKKGPGMA 2206
G1 (ants) KAALKAAMQ
AP00377 P82415, Ponericin GWKDWLKKGKEWLKAKGPGIVK 2207
G2 (ants) AALQAATQ
AP00378 P82416, Ponericin GWKDWLNKGKEWLKKKGPGIMK 2208
G3 (ants) AALKAATQ
AP00379 P82417, Ponericin DFKDWMKTAGEWLKKKGPGILKA 2209
G4 (ants) AMAAAT
AP00380 P82418, Ponericin GLKDWVKIAGGWLKKKGPGILKA 2210
G5 (ants) AMAAATQ
AP00381 P82419, Ponericin GLVDVLGKVGGLIKKLLP 2211
G6 (ants)
AP00382 P82420, Ponericin GLVDVLGKVGGLIKKLLPG 2212
G7 (ants)
AP00383 P82421, Ponericin LLKELWTKMKGAGKAVLGKIKGLL 2213
L1 (ants)
AP00384 P82422, Ponericin LLKELWTKIKGAGKAVLGKIKGLL 2214
L2 (ants)
AP00386 P82423, Ponericin WLGSALKIGAKLLPSVVGLFKKKKQ 2215
W1 (ants)
AP00387 P82424, Ponericin WLGSALKIGAKLLPSVVGLFQKKKK 2216
W2 (ants)
AP00388 P82425, Ponericin GIWGTLAKIGIKAVPRVISMLKKK 2217
W3 (ants) KQ
AP00389 P82426, Ponericin GIWGTALKWGVKLLPKLVGMAQT 2218
W4 (ants) KKQ
AP00390 P82427, Ponericin FWGALIKGAAKLIPSVVGLFKKKQ 2219
W5 (ants)
AP00391 P82428, Ponericin FIGTALGIASAIPAIVKLFK 2220
W6 (ants)
AP00303 P82651, Tigerinin- FCTMIPIPRCY 2221
1 (frog)
AP00304 P82652, Tigerinin- RVCFAIPLPICH 2222
2 (frog)
AP00305 P82653, Tigerinin- RVCYAIPLPICY 2223
3 (frog)
AP00301 P82656, Hadrurin GILDTIKSIASKVWNSKTVQDLKR 2224
(scorpion) KGINWVANKLGVSPQAA
AP00113 P82740, GLLSGLKKVGKHVAKNVAVSLMD 2225
RANATUERIN 1T SLKCKISGDC
(frog)
AP00114 P82741, SMLSVLKNLGKVGLGFVACKINK 2226
RANATUERIN 1 QC
(Ranatuerin-1,
frog)
AP00115 P82742, GLFLDTLKGAAKDVAGKLEGLKC 2227
RANATUERIN 2 KITGCKLP
(Ranatuerin-2,
frog)
AP00116 P82780, GFLDIINKLGKTFAGHMLDKIKCTI 2228
RANATUERIN 3 GTCPPSP
(Ranatuerin-3,
frog)
AP00117 P82819, FLPFIARLAAKVFPSIICSVTKKC 2229
RANATUERIN 4
(Ranatuerin-4,
frog)
AP00405 P82821, FISAIASMLGKFL 2230
RANATUERIN 6
(frog)
AP00406 P82822, FLSAIASMLGKFL 2231
RANATUERIN 7
(frog)
AP00407 P82823, FISAIASFLGKFL 2232
RANATUERIN 8
(frog)
AP00408 P82824, FLFPLITSFLSKVL 2233
RANATUERIN 9
(frog)
AP00461 P82825, Brevinin- FLPMLAGLAASMVPKLVCLITKKC 2234
1LA (frog)
AP00462 P82826, Brevinin- FLPMLAGLAASMVPKFVCLITKKC 2235
1LB (frog)
AP00118 P82828, GILDSFKGVAKGVAKDLAGKLLD 2236
RANATUERIN KLKCKITGC
2La (Ranatuerin-
2La, frog)
AP00119 P82829, GILSSIKGVAKGVAKNVAAQLLDT 2237
RANATUERIN LKCKITGC
2Lb (Ranatuerin-
2Lb, frog)
AP00109 P82830, Temporin- VLPLISMALGKLL 2238
1La (Temporin
1La, frog)
AP00110 P82831, Temporin- NFLGTLINLAKKIM 2239
1Lb (Temporin
1Lb, frog)
AP00111 P82832, Temporin- FLPILINLIHKGLL 2240
1Lc (Temporin
1Lc, frog)
AP00463 P82833, Brevinin- FLPFIAGMAAKFLPKIFCAISKKC 2241
1BA (frog)
AP00464 P82834, Brevinin- FLPAIAGMAAKFLPKIFCAISKKC 2242
1BB (frog)
AP00465 P82835, Brevinin- FLPFIAGVAAKFLPKIFCAISKKC 2243
1BC (frog)
AP00466 P82836, Brevinin- FLPAIAGVAAKFLPKIFCAISKKC 2244
1BD (frog)
AP00467 P82837, Brevinin- FLPAIVGAAAKFLPKIFCVISKKC 2245
1BE (frog)
AP00468 P82838, Brevinin- FLPFIAGMAANFLPKIFCAISKKC 2246
1BF (frog)
AP00120 P82840, GLLDTIKGVAKTVAASMLDKLKC 2247
RANATUERIN 2B KISGC
(Ranatuerin-2B,
frog)
AP00469 P82841, Brevinin- FLPIIAGVAAKVFPKIFCAISKKC 2248
1PA (frog)
AP00460 P82842, Brevinin- FLPIIAGIAAKVFPKIFCAISKKC 2249
1PB (frog)
AP00470 P82843, Brevinin- FLPIIASVAAKVFSKIFCAISKKC 2250
1PC (frog)
AP00471 P82844, Brevinin- FLPIIASVAANVFSKIFCAISKKC 2251
1PD (frog)
AP00472 P82845, Brevinin- FLPIIASVAAKVFPKIFCAISKKC 2252
1PE (frog)
AP00121 P82847, GLMDTVKNVAKNLAGHMLDKLK 2253
RANATUERIN 2P CKITGC
(Ranatuerin-2P,
frog)
AP00112 P82848, Temporin- FLPIVGKLLSGLL 2254
1P (Temporin 1P,
frog)
AP00452 P82871, Brevinin- FLPVVAGLAAKVLPSIICAVTKKC 2255
1SY (frog)
AP00122 P82875, SMLSVLKNLGKVGLGLVACKINK 2256
Ranatuerin-1C QC
(Ranatuerin 1C,
frog)
AP00514 P82876, Ranalexin- FLGGLMKAFPALICAVTKKC 2257
1Ca (frog)
AP00515 P82877, Ranalexin- FLGGLMKAFPAIICAVTKKC 2258
1Cb (frog)
AP00124 P82878, GLFLDTLKGAAKDVAGKLLEGLK 2259
Ranatuerin-2Ca CKIAGCKP
(Ranatuerin 2Ca,
frog)
AP00123 P82879, GLFLDTLKGLAGKLLQGLKCIKAG 2260
Ranatuerin-2Cb CKP
(Ranatuerin 2Cb,
frog)
AP00104 P82880, Temporin- FLPFLAKILTGVL 2261
1Ca (Temporin
1Ca, frog)
AP00105 P82881, Temporin- FLPLFASLIGKLL 2262
1Cb (Temporin
1Cb, frog)
AP00106 P82882, Temporin- FLPFLASLLTKVL 2263
1Cc (Temporin
1Cc, frog)
AP00107 P82883, Temporin- FLPFLASLLSKVL 2264
1Cd (Temporin
1Cd, frog)
AP00108 P82884, Temporin- FLPFLATLLSKVL 2265
1Ce (Temporin
1Ce, frog)
AP00453 P82904, Brevinin- FLPAIVGAAGQFLPKIFCAISKKC 2266
1SA (frog)
AP00454 P82905, Brevinin- FLPAIVGAAGKFLPKIFCAISKKC 2267
1SB (frog)
AP00455 P82906, Brevinin- FFPIVAGVAGQVLKKIYCTISKKC 2268
1SC (frog)
AP00996 P82907, Lichenin ISLEICAIFHDN 2269
(bacteria)
AP00302 P82951, Hepcidin GCRFCCNCCPNMSGCGVCCRF 2270
(fish)
AP00058 P83080, Maximin 1 GIGTKILGGVKTALKGALKELAST 2271
(toad) YAN
AP00059 P83081, Maximin 2 GIGTKILGGVKTALKGALKELAST 2272
(toad) YVN
AP00060 P83082, Maximin 3 GIGGKILSGLKTALKGAAKELAST 2273
(toad, ZZHa) YLH
AP00061 P83083, Maximin 4 GIGGVLLSAGKAALKGLAKVLAE 2274
(toad) KYAN
AP00062 P83084, Maximin 5 SIGAKILGGVKTFFKGALKELASTY 2275
(toad) LQ
AP00063 P83085, Maximin 6 ILGPVISTIGGVLGGLLKNL 2276
(toad)
AP00064 P83086, Maximin 7 ILGPVLGLVGNALGGLIKNE 2277
(toad)
AP00065 P83087, Maximin 8 ILGPVLSLVGNALGGLLKNE 2278
(toad)
AP00355 P83171, ANTAFVSSAHNTQKIPAGAPFNRN 2279
Ginkbilobin LRAMLADLRQNAAFAG
(Chinese plant)
AP00475 P83188, Pseudin 1 GLNTLKKVFQGLHEAIKLINNHVQ 2280
(frog)
AP00476 P83189, Pseudin 2 GLNALKKVFQGIHEAIKLINNHVQ 2281
(frog)
AP00477 P83190, Pseudin 3 GINTLKKVIQGLHEVIKLVSNHE 2282
(frog)
AP00478 P83191, Pseudin 4 GINTLKKVIQGLHEVIKLVSNHA 2283
(frog)
AP00410 P83287, SKGKKANKDVELARG 2284
Oncorhyncin III
(fish)
AP00357 P83305, Japonicin- FFPIGVFCKIFKTC 2285
1 (amphibian, frog)
AP00358 P83306, Japonicin- FGLPMLSILPKALCILLKRKC 2286
2 (amphibian, frog)
AP00385 P83312, FKLGSFLKKAWKSKLAKKLRAKG 2287
Parabutoporin KEMLKDYAKGLLEGGSEEVPGQ
(scorpion)
AP00374 P83313, GKVWDWIKSTAKKLWNSEPVKEL 2288
Opistoporin 1 KNTALNAAKNLVAEKIGATPS
(scorpion)
AP00375 P83314, GKVWDWIKSTAKKLWNSEPVKEL 2289
Opistoporin 2 KNTALNAAKNFVAEKIGATPS
(scorpion)
AP00336 P83327, Histone AERVGAGAPVYL 2290
H2A (fish)
AP00335 P83338, Histone PKRKSATKGDEPA 2291
H6-like protein
(fish)
AP00411 P83374, KAVAAKKSPKKAKKPAT 2292
Oncorhyncin II
(fish)
AP00999 P83375, Serracin-P DYHHGVRVL 2293
43 kDa subunit
(bacteria)
AP00284 P83376, SHQDCYEALHKCMASHSKPFSCS 2294
Dolabellanin B2 MKFHMCLQQQ
(sea hare)
AP00998 P83378, Serracin-P ALPKKLKYLNLFNDGFNYMGVV 2295
23 kDa subunit
(bacteriocin,
bacteria)
AP00129 P83403, Cecropin GWLKKIGKKIERVGQNTRDATVK 2296
(insect, moth) GLEVAQQAANVAATVR
AP00127 P83413, Cecropin RWKVFKKIEKVGRNIRDGVIKAAP 2297
A (insect, moth) AIEVLGQAKAL
AP00372 P83416, Virescein GKIPIGAIKKAGKAIGKGLRAVNIA 2298
(insect) STAHDVYTFFKPKKRH
AP00356 P83427, Heliocin QRFIHPTYRPPPQPRRPVIMRA 2299
(insect)
AP00409 P83428, Locustin ATTGCSCPQCIIFDPICASSYKNGRR 2300
(insect) GFSSGCHMRCYNRCHGTDYFQISK
GSKCI
AP00339 P83545, FFGWLIKGAIHAGKAIHGLIHRRRH 2301
Chrysophsin-1
(Red sea bream,
madai)
AP00340 P83546, FFGWLIRGAIHAGKAIHGLIHRRRH 2302
Chrysophsin-2
(Red sea bream,
madai)
AP00341 P83547, FIGLLISAGKAIHDLIRRRH 2303
Chrysophsin-3
(Red sea bream,
madai)
AP01004 P84763, Thuricin-S DWTAWSALVAAACSVELL 2304
(bacteria)
AP00553 P84868, Sesquin KTCENLADTY 2305
(plant, ZZHp)
AP00132 Q06589, Cecropin GWLKKIGKKIERVGQHTRDATIQTI 2306
1 (insect, fly) AVAQQAANVAATAR
AP00135 Q06590, Cecropin GWLKKIGKKIERVGQHTRDATIQTI 2307
2 (insect fly) GVAQQAANVAATLK
AP00416 Q17313, SLGGVISGAKKVAKVAIPIGKAVLP 2308
Ceratotoxin C VVAKLVG
(insect, fly)
AP00171 Q24395, HRHQGPIFDTRPSPFNPNQPRPGPIY 2309
Metchnikowin
(insect)
AP00354 Q27023, Tenecin 1 VTCDILSVEAKGVKLNDAACAAH 2310
(insect) CLFRGRSGGYCNGKRVCVCR
AP00401 Q28880, Lingual GFTQGVRNSQSCRRNKGICVPIRCP 2311
antimicrobial GSMRQIGTCLGAQVKCCRRK
peptide (LAP, beta
defensin, cow)
AP00224 Q62713, RatNP-3 CSCRTSSCRFGERLSGACRLNGRIY 2312
(rat) RLCC
AP00225 Q62714, RatNP-4 ACYCRIGACVSGERLTGACGLNGR 2313
(rat) IYRLCCR
AP00223 Q62715, RatNP-2 VTCYCRSTRCGFRERLSGACGYRG 2314
(rat) RIYRLCCR
AP00222 Q62716, RatNP-1 VTCYCRRTRCGFRERLSGACGYRG 2315
(rat) RIYRLCCR
AP00174 Q64365, GNCP-1 RRCICTTRTCRFPYRRLGTCIFQNR 2316
(Guinea pig VYTFCC
neutrophil cationic
peptide 1)
AP00311 Q90W78, Galensin CYSAAKYPGFQEFINRKYKSSRF 2317
(frog)
AP00395 Q95NT0, HSSGYTRPLPKPSRPIFIRPIGCDVC 2318
Penaeidin-4a YGIPSSTARLCCFRYGDCCHR
(shrimp, Crustacea)
AP00423 Q962B0, QGYKGPYTRPILRPYVRPVVSYNA 2319
Penaeidin-3n CTLSCRGITTTQARSCSTRLGRCCH
(shrimp, Crustacea) VAKGYS
AP00422 Q962B1, QGCKGPYTRPILRPYVRPVVSYNA 2320
Penaeidin-3m CTLSCRGITTTQARSCCTRLGRCCH
(shrimp, Crustacea) VAKGYS
AP00421 Q963C3, YSSGYTRPLPKPSRPIFIRPIGCDVC 2321
Penaeidin-4C YGIPSSTARLCCFRYGDCCHR
(shrimp, Crustacea)
AP00210 Q99134, PGLa GMASKAGAIAGKIAKVALKAL 2322
(African clawed
frog, XXA)
AP00054 Q9DET7, GIGGALLSAGKSALKGLAKGLAEH 2323
Bombinin-like FAN
peptide 7 (BLP-7,
toad)
AP00315 Q9PT75, SLGSFLKGVGTTLASVGKVVSDQF 2324
Dermatoxin (Two- GKLLQAGQ
colored leaf frog)
AP00133 Q9Y0Y0, Cecropin GGLKKLGKKLEGVGKRVFKASEK 2325
B (insect, ALPVLTGYKAIG
mosquito)
AP00004 Ref, Ct-AMP1 NLCERASLTWTGNCGNTGHCDTQ 2326
(CtAMP1, C. CRNWESAKHGACHKRGNWKCFC
ternatea- YFDC
antimicrobial
peptide 1, plant
defensin)
AP00027 Ref, hexapeptide RRWQWR 2327
(synthetic)
AP00529 Ref, Lantibiotic WKSESVCTPGCVTGVLQTCFLQTI 2328
Ericin S (bacteria) TCNCHISK
AP00306 Ref, Tigerinin-4 RVCYAIPLPIC 2329
(frog)
AP00309 Ref, Human KS-27 KSKEKIGKEFKRIVQRIKDFLRNLV 2330
(KS27 from LL-37) PR
AP00344 Ref, Apidaecin II GNNRPIYIPQPRPPHPRL 2331
(honeybee, insect)
AP00424 Ref, XT1 (frog) GFLGPLLKLAAKGVAKVIPHLIPSR 2332
QQ
AP00425 Ref, XT 2 (frog) GCWSTVLGGLKKFAKGGLEAIVNPK 2333
AP00426 Ref, XT 4 (frog) GVFLDALKKFAKGGMNAVLNPK 2334
AP00427 Ref, XT 7 (frog) GLLGPLLKIAAKVGSNLL 2335
AP00431 Ref, human LLP 1 RVIEVVQGACRAIRHIPRRIRQGLE 2336
RIL
AP00432 Ref, human LLP RIAGYGLRGLAVIIRICIRGLNLIFEI 2337
IR
AP00447 Ref, Anoplin GLLKRIKTLL 2338
(insect)
AP00474 Ref, Piscidin 3 FIHHIFRGIVHAGRSIGRFLTG 2339
(fish)
AP00481 Ref, Kaliocin-1 FFSASCVPGADKGQFPNLCRLCAG 2340
(synthetic) TGENKCA
AP00482 Ref, Thionin KSCCRNTWARNCYNVCRLPGTISR 2341
mutation EICAKKCRCKIISGTTCPSDYPK
(synthetic)
AP00484 Ref, Stomoxyn RGFRKHFNKLVKKVKHTISETAHV 2342
(insect, fly) AKDTAVIAGSGAAVVAAT
AP00486 Ref, Cupiennin 1b GFGSLFKFLAKKVAKTVAKQAAK 2343
(spider) QGAKYIANKQME
AP00487 Ref, Cupiennin 1c GFGSLFKFLAKKVAKTVAKQAAK 2344
(spider) QGAKYIANKQTE
AP00488 Ref, Cupiennin 1D GFGSLFKFLAKKVAKTVAKQAAK 2345
(spider) QGAKYVANKHME
AP00489 Ref, Hipposin SGRGKTGGKARAKAKTRSSRAGL 2346
(fish) QFPVGRVHRLLRKGNYAHRVGAG
APVYL
AP00923 Ref, AISYGNGVYCNKEKCWVNKAENK 2347
Carnobacteriocin QAITGIVIGGWASSLAGMGH
B1 (XXO, class IIa
bacteriocin,
bacteria)
AP00496 Ref, HP 2-20 AKKVFKRLEKLFSKIQNDK 2348
(synthetic)
AP00497 Ref, Maximin H5 ILGPVLGLVSDTLDDVLGIL 2349
(toad)
AP00498 Ref, rCRAMP (rat GLVRKGGEKFGEKLRKIGQKIKEF 2350
cathelicidin) FQKLALEIEQ
AP00500 Ref, S9-P18 KWKLFKKISKFLHLAKKF 2351
(synthetic)
AP00501 Ref, L9-P18 KWKLFKKILKFLHLAKKF 2352
(synthetic)
AP00502 Ref, Clavaspirin FLRFIGSVIHGIGHLVHHIGVAL 2353
(sea squirt,
tunicate)
AP00503 Ref, human P- AKRHHGYKRKFH 2354
113D
AP00504 Ref, human MUC7 LAHQKPFIRKSYKCLHKRCR 2355
20-Mer
AP00507 Ref, Nigrocin 2 GLLSKVLGVGKKVLCGVSGLC 2356
(frog)
AP00508 Ref, Nigrocin 1 GLLDSIKGMAISAGKGALQNLLKV 2357
(frog) ASCKLDKTC
AP00509 Ref, human VAIALKAAHYHTHKE 2358
Calcitermin
AP00510 Ref, Dicynthaurin ILQKAVLDCLKAAGSSLSKAAITAI 2359
(sea peach) YNKIT
AP00511 Ref, KIGAKI KIGAKIKIGAKIKIGAKI 2360
(synthetic)
AP00516 Ref, Lycotoxin I IWLTALKFLGKHAAKHLAKQQLS 2361
(spider) KL
AP00517 Ref, Lycotoxin II KIKWFKTMKSIAKFIAKEQMKKHL 2362
(spider) GGE
AP00518 Ref, Ib-AMP3 QYRHRCCAWGPGRKYCKRWC 2363
(plant defensin,
balsam)
AP00519 Ref, Ib-AMP4 EWGRRCCGWGPGRRYCRRWC 2364
(plant defensin,
balsam)
AP00521 Ref, Dhvar4 KRLFKKLLFSLRKY 2365
(synthetic)
AP00522 Ref, Dhvar5 LLLFLLKKRKKRKY 2366
(synthetic)
AP00525 Ref, Maximin H2 ILGPVLSMVGSALGGLIKKI 2367
(toad)
AP00526 Ref, Maximin H3 ILGPVLGLVGNALGGLIKKI 2368
(toad)
AP00527 Ref, Maximin H4 ILGPVISKIGGVLGGLLKNL 2369
(toad)
AP00528 Ref, Anionic DDDDDD 2370
peptide SAAP
(sheep)
AP00530 Ref, Lantibiotic VLSKSLCTPGCITGPLQTCYLCFPT 2371
Ericin A (bacteria) FAKC
AP00531 Ref, Kenojeinin I GKQYFPKVGGRLSGKAPLAAKTH 2372
(sea skate) RRLKP
AP00532 Ref, Lunatusin KTCENLADTFRGPCFATSNC 2373
(plant, ZZHp)
AP00533 Ref, Fallaxin (frog) GVVDILKGAAKDIAGHLASKVMN 2374
KL
AP00534 Ref, Tu-AMP 2 KSCCRNTTARNCYNVCRIPG 2375
(TuAMP2, thionin-
like antimicrobial
peptides, plant
defensin, tulip)
AP00535 Ref, Pilosulin 1 GLGSVFGRLARILGRVIPKVAKKL 2376
(Myr b I) GPKVAKVLPKVMKEAIPMAVEMA
(Australian ants) KSQEEQQPQ
AP00536 Ref, Luxuriosin SVRTQDNAVNRQIFGSNGPYRDFQ 2377
(insect) LSDCYLPLETNPYCNEWQFAYHW
NNALMDCERAIYHGCNRTRNNFIT
LTACKNQAGPICNRRRH
AP00537 Ref, SAMP H1 AEVAPAPAAAAPAKAPKKKAAAK 2378
(fish, Atlantic PKKAGPS
salmon)
AP00538 Ref, Halocidin WLNALLHHGLNCAKGVLA 2379
(dimer Hal18 +
Hal15) (tunicate)
AP00539 Ref, AOD GFGCPWNRYQCHSHCRSIGRLGGY 2380
(American oyster CAGSLRLTCTCYRS
defensin, animal
defensin)
AP00540 Ref, Pentadactylin GLLDTLKGAAKNVVGSLASKVME 2381
(frog) KL
AP00541 Ref, Polybia-MPI IDWKKLLDAAKQIL 2382
(insect, social
wasp)
AP00542 Ref, Polybia-CP ILGTILGLLKSL 2383
(insect, social
wasp)
AP00543 Ref, Ocellatin-1 GVVDILKGAGKDLLAHLVGKISEKV 2384
(XXA, frog)
AP00544 Ref, Ocellatin-2 GVLDIFKDAAKQILAHAAEKQI 2385
(XXA, frog)
AP00545 Ref, Ocellatin-3 GVLDILKNAAKNILAHAAEQI 2386
(frog)
AP00548 Ref, CMAP 27 RFGRFLRKIRRFRPKVTITIQGSARFG 2387
(chicken myeloid
antimicrobial
peptide 27, bird
cathelicidin,
chicken
cathelicidin)
AP00550 Ref, Tu-AMP-1 KSCCRNTVARNCYNVCRIPGTPRP 2388
(TuAMP1, thionin- VCAATCDCKLITGTKCPPGYEK
like antimicrobial
peptides, plant
defensin, tulip)
AP00551 Ref, Combi-2 FRWWHR 2389
(synthetic)
AP00552 Ref, Maximin 9 GIGRKFLGGVKTTFRCGVKDFASK 2390
(frog) HLY
AP00554 Ref, Sl moricin GKIPVKAIKKAGAAIGKGLRAINIA 2391
(insect) STAHDVYSFFKPKHKKK
AP00555 Ref, Parasin I KGRGKQGGKVRAKAKTRSS 2392
(catfish)
AP00556 Ref, Kassinatuerin- GFMKYIGPLIPHAVKAISDLI 2393
1 (frog)
AP00557 Ref, Fowlicidin-1 RVKRVWPLVIRTVIAGYNLYRAIK 2394
(chCATH-1, bird KK
cathelicidin,
chicken
cathelicidin)
AP00559 Ref, Eryngin ATRVVYCNRRSGSVVGGDDTVYY 2395
(mushroom, fungi) EG
AP00560 Ref, Dendrocin TTLTLHNLCPYPVWWLVTPNNGG 2396
(plant, bamboo) FPIIDNTPVVLG
AP00561 Ref, Coconut EQCREEEDDR 2397
antifungal peptide
(plant)
AP00562 Ref, Pandinin 1 GKVWDWIKSAAKKIWSSEPVSQL 2398
(African scorpion) KGQVLNAAKNYVAEKIGATPT
AP00563 Ref, White cloud KTCENLADTFRGPCFATSNCDDHC 2399
bean defensin KNKEHLLSGRCRDDFRCWCTRNC
(plant defensin)
AP00564 Ref, Dybowskin-1 FLIGMTHGLICLISRKC 2400
(frog)
AP00565 Ref, Dybowskin-2 FLIGMTQGLICLITRKC 2401
(frog)
AP00566 Ref, Dybowskin-3 GLFDVVKGVLKGVGKNVAGSLLE 2402
(frog) QLKCKLSGGC
AP00567 Ref, Dybowskin-4 VWPLGLVICKALKIC 2403
(frog)
AP00568 Ref, Dybowskin-5 GLFSVVTGVLKAVGKNVAKNVGG 2404
(frog) SLLEQLKCKKISGGC
AP00569 Ref, Dybowskin-6 FLPLLLAGLPLKLCFLFKKC 2405
(frog)
AP00570 Ref, Pleurain-A1 SIITMTKEAKLPQLWKQIACRLYNTC 2406
(frog)
AP00571 Ref, Pleurain-A2 SIITMTKEAKLPQSWKQIACRLYNTC 2407
(frog)
AP00574 Ref, Esculentin- GLFSKFAGKGIKNLIFKGVKHIGKE 2408
IGRa (frog) VGMDVIRTGIDVAGCKIKGEC
AP00575 Ref, Brevinin- GLLDTFKNLALNAAKSAGVSVLNS 2409
2GRa (frog) LSCKLSKTC
AP00576 Ref, Brevinin- GVLGTVKNLLIGAGKSAAQSVLKT 2410
2GRb (frog) LSCKLSNDC
AP00577 Ref, Brevinin- GLFTLIKGAAKLIGKTVAKEAGKT 2411
2GRc (frog) GLELMACKITNQC
AP00578 Ref, Brevinin- FLPLLAGLAANFLPKIFCKITKKC 2412
1GRa (frog)
AP00579 Ref, Nigrocin- GLLSGILGAGKHIVCGLSGLC 2413
2GRa (frog)
AP00580 Ref, Nigrocin- GLFGKILGVGKKVLCGLSGMC 2414
2GRb (frog)
AP00581 Ref, Nigrocin- GLLSGILGAGKNIVCGLSGLC 2415
2GRc (frog)
AP00582 Ref, Brevinin- GFSSLFKAGAKYLLKSVGKAGAQ 2416
2GHa (frog) QLACKAANNCA
AP00583 Ref, Brevinin- GVITDALKGAAKTVAAELLRKAH 2417
2GHb (frog) CKLTNSC
AP00584 Ref, Guentherin VIDDLKKVAKKVRRELLCKKHHK 2418
(frog) KLN
AP00585 Ref, Brevinin- SIWEGIKNAGKGFLVSILDKVRCK 2419
2GHc (frog) VAGGCNP
AP00586 Ref, Temporin-GH FLPLLFGAISHLL 2420
(frog)
AP00587 Ref, Brevinin-2TSa GIMSLFKGVLKTAGKHVAGSLVD 2421
(frog) QLKCKITGGC
AP00588 Ref, Brevinin-1TSa FLGSIVGALASALPSLISKIRN 2422
(frog)
AP00589 Ref, Temporin- FLGALAKIISGIF 2423
1TSa (frog)
AP00593 Ref, Brevinin-1CSa FLPILAGLAAKIVPKLFCLATKKC 2424
(frog)
AP00594 Ref, Temporin- FLPIVGKLLSGLL 2425
1CSa (frog)
AP00595 Ref, Temporin- FLPIIGKLLSGLL 2426
1CSb (frog)
AP00596 Ref, Temporin- FLPLVTGLLSGLL 2427
1CSc (frog)
AP00597 Ref, Temporin- NFLGTLVNLAKKIL 2428
1CSd (frog)
AP00598 Ref, Temporin- FLSAITSLLGKLL 2429
1SPb (frog)
AP00599 Ref, Brevinin-2- GIWDTIKSMGKVFAGKILQNL 2430
related (frog)
AP00600 Ref, Odorranain- GLLRASSVWGRKYYVDLAGCAKA 2431
HP (frog)
AP00601 Ref, Brevinin- FLSLALAALPKFLCLVFKKC 2432
1DYa (frog)
AP00602 Ref, Brevinin- FLSLALAALPKLFCLIFKKC 2433
1DYb (frog)
AP00603 Ref, Brevinin- FLPLLLAGLPKLLCLFFKKC 2434
1DYc (frog)
AP00607 Ref, Brevinin- GLFDVVKGVLKGAGKNVAGSLLE 2435
2DYb (frog) QLKCKLSGGC
AP00608 Ref, Brevinin- GLFDVVKGVLKGVGKNVAGSLLE 2436
2DYc (frog) QLKCKLSGGC
AP00609 Ref, Brevinin- GIFDVVKGVLKGVGKNVAGSLLE 2437
2DYd (frog) QLKCKLSGGC
AP00610 Ref, Brevinin- GLFSVVTGVLKAVGKNVAKNVGG 2438
2DYe (frog) SLLEQLKCKISGGC
AP00611 Ref, Temporin- FIGPIISALASLFG 2439
1DYa (frog)
AP00615 Ref, Palustrin-1b ALFSILRGLKKLGNMGQAFVNCKI 2440
(frog) YKKC
AP00616 Ref, Palustrin-1c ALSILRGLEKLAKMGIALTNCKAT 2441
(frog) KKC
AP00617 Ref, Palustrin-1d ALSILKGLEKLAKMGIALTNCKAT 2442
(frog) KKC
AP00619 Ref, Palustrin-2b GFFSTVKNLATNVAGTVIDTLKCK 2443
(frog) VTGGCRS
AP00620 Ref, Palustrin-2c GFLSTVKNLATNVAGTVIDTLKCK 2444
(frog) VTGGCRS
AP00621 Ref, Palustrin-3a GIFPKIIGKGIKTGIVNGIKSLVKGV 2445
(frog) GMKVFKAGLNNIGNTGCNEDEC
AP00622 Ref, Palustrin-3b GIFPKIIGKGIKTGIVNGIKSLVKGV 2446
(frog) GMKVFKAGLSNIGNTGCNEDEC
AP00624 Ref, human ALL- ALLGDFFRKSKEKIGKEFKRIVQRI 2447
38 (an LL-37 KDFLRNLVPRTES
analog released
from its precursor
hCAP-18 by
gastricsin in vivo)
AP00625 Ref, human KR-20 KRIVQRIKDFLRNLVPRTES 2448
(KR20 from LL-
37)
AP00626 Ref, human KS-30 KSKEKIGKEFKRIVQRIKDFLRNLV 2449
(KS30 from LL-37) PRTES
AP00627 Ref, human RK-31 RKSKEKIGKEFKRIVQRIKDFLRNL 2450
(RK31 from LL- VPRTES
37)
AP00628 Ref, human LL-23 LLGDFFRKSKEKIGKEFKRIVQR 2451
(LL23 from LL-37)
AP00629 Ref, human LL-29 LLGDFFRKSKEKIGKEFKRIVQRIK 2452
(LL29 from LL-37) DFLR
AP00630 Ref, Amoeba GEILCNLCTGLINTLENLLTTKGAD 2453
peptide (protozoan
para
AP00631 Ref, Mundticin KYYGNGVSCNKKGCSVDWGKAIG 2454
(bacteria) IIGNNSAANLATGGAAGWSK
AP00638 Ref, Citropin 2.1 GLIGSIGKALGGLLVDVLKPKL 2455
(frog)
AP00639 Ref, Citropin 2.1.3 GLIGSIGKALGGLLVDVLKPKLQA 2456
(frog) AS
AP00640 Ref, Maculatin 1.3 GLLGLLGSVVSHVVPAIVGHF 2457
(frog)
AP00641 Ref, Pardaxin 1 GFFALIPKIISSPLFKTLLSAVGSALS 2458
(Pardaxin P-1, SSGEQE
Pardaxin P1, Pa1,
flat fish)
AP00642 Ref, Pardaxin 2 GFFALIPKIISSPIFKTLLSAVGSALS 2459
(Pardaxin P-2, SSGGQE
Pardaxin P2, Pa2,
flat fish)
AP00643 Ref, Pardaxin 3 GFFAFIPKIISSPLFKTLLSAVGSALS 2460
(Pardaxin P-3, SSGEQE
Pardaxin P3, Pa3,
flat fish)
AP00645 Ref, Pardaxin 5 GFFAFIPKIISSPLFKTLLSAVGSALS 2461
(Pardaxin P-5, SSGDQE
Pardaxin P5, Pa5,
flat fish)
AP00647 Ref, Brevinin-1PLb FLPLIAGLAANFLPKIFCAITKKC 2462
(frog)
AP00648 Ref, Brevinin-1PLc FLPVIAGVAAKFLPKIFCAITKKC 2463
(frog)
AP00649 Ref, Esculentin- GLFPKINKKKAKTGVFNIIKTVGKE 2464
1PLa (frog) AGMDLIRTGIDTIGCKIKGEC
AP00650 Ref, Esculentin- GIFTKINKKKAKTGVFNIIKTIGKEA 2465
1PLb (frog) GMDVIRAGIDTISCKIKGEC
AP00651 Ref, Esculentin- GLFSILKGVGKIALKGLAKNMGK 2466
2PLa (frog) MGLDLVSCKISKEC
AP00652 Ref, Ranatuerin- GIMDTVKNVAKNLAGQLLDKLKC 2467
2PLa (frog) KITAC
AP00653 Ref, Ranatuerin- GIMDTVKNAAKDLAGQLLDKLKC 2468
2PLb (frog) RITGC
AP00654 Ref, Ranatuerin- GLLDTIKNTAKNLAVGLLDKIKCK 2469
2PLc (frog) MTGC
AP00655 Ref, Ranatuerin- GIMDSVKNVAKNIAGQLLDKLKC 2470
2PLd (frog) KITGC
AP00656 Ref, Ranatuerin- GIMDSVKNAAKNLAGQLLDTIKCK 2471
2PLe (frog) ITAC
AP00657 Ref, Ranatuerin- GIMDTVKNAAKDLAGQLDKLKCR 2472
2PLf (frog) ITGC
AP00658 Ref, Temporin- FLPLVGKILSGLI 2473
1PLa (frog)
AP00659 Ref, Ranatuerin 5 FLPIASLLGKYL 2474
(frog)
AP00661 Ref, Esculentin-2L GILSLFTGGIKALGKTLFKMAGKA 2475
(frog) GAEHLACKATNQC
AP00662 Ref, Esculentin-2B GLFSILRGAAKFASKGLGKDLTKL 2476
(ESC2B-RANBE, GVDLVACKISKQC
frog)
AP00663 Ref, Esculentin-2P GFSSIFRGVAKFASKGLGKDLARL 2477
(frog) GVNLVACKISKQC
AP00664 Ref, Peptide A1 FLPAIAGILSQLF 2478
(frog)
AP00665 Ref, Peptide B9 FLPLIAGLIGKLF 2479
(frog)
AP00666 Ref, PG-L ( frog) EGGGPQWAVGHFM 2480
AP00667 Ref, PG-KI (frog) EPHPDEFVGLM 2481
AP00668 Ref, PG-KII (frog) EPNPDEFVGLM 2482
AP00669 Ref, PG-KIII (frog) EPHPNEFVGLM 2483
AP00670 Ref, PG-SPI (frog) EPNPDEFFGLM 2484
AP00660 Ref, Pandinin 2 FWGALAKGALKLIPSLFSSFSKKD 2485
(African scorpion)
AP00671 Ref, PG-SPII (frog) EPNPNEFFGLM 2486
AP00673 Ref, Lantibiotic WKSESVCTPGCVTGVLQTCFLQTI 2487
Ericin S (bacteria TCNCHISK
AP00674 Ref, Lantibiotic VLSKSLCTPGCITGPLQTCYLCFPT 2488
Ericin A (bacteria FAKC
AP00675 Ref, Human beta FELDRICGYGTARCRKKCRSQEYRI 2489
defensin 4 (HBD-4, GRCPNTYACCLRKWDESLLNRTKP
HBD4, human
defensin)
AP00676 Ref, RL-37 (RL37, RLGNFFRKVKEKIGGGLKKVGQKI 2490
monkey KDFLGNLVPRTAS
cathelicidin)
AP00677 Ref, CAP11 GLRKKFRKTRKRIQKLGRKIGKTG 2491
(Guinea pig RKVWKAWREYGQIPYPCRI
cathelicidin)
AP00678 Ref, Canine RLKELITTGGQKIGEKIRRIGQRIKD 2492
cathelicidin FFKNLQPREEKS
(K9CATH) (dog)
AP00679 Ref, Esculentin GLFSILKGVGKIAIKGLGKNLGKM 2493
2VEb (frog) GLDLVSCKISKEC
AP00680 Ref, SMAP-34 GLFGRLRDSLQRGGQKILEKAERI 2494
(sheep cathelicidin) WCKIKDIFR
AP00681 Ref, OaBac5 RFRPPIRRPPIRPPFRPPFRPPVRPPIR 2495
(sheep cathelicidin) PPFRPPFRPPIGPFP
AP00682 Ref, OaBac6 RRLRPRHQHFPSERPWPKPLPLPLP 2496
(sheep cathelicidin) RPGPRPWPKPLPLPLPRPGLRPWPK
PL
AP00683 Ref, OaBac7.5 RRLRPRRPRLPRPRPRPRPRPRSLPL 2497
(sheep cathelicidin) PRPQPRRIPRPILLPWRPPRPIPRPQI
QPIPRWL
AP00684 Ref, OaBac11 RRLRPRRPRLPRPRPRPRPRPRSLPL 2498
(sheep cathelicidin) PRPKPRPIPRPLPLPRPRPKPIPRPLP
LPRPRPRRIPRPLPLPRPRPRPIPRPL
PLPQPQPSPIPRPL
AP00685 Ref, Ranatuerin GIMDTVKGVAKTVAASLLDKLKC 2499
2VEb (frog) KITGC
AP00686 Ref, eCATH-1 KRFGRLAKSFLRMRILLPRRKILLAS 2500
(horse cathelicidin)
AP00687 Ref, eCATH-2 KRRHWFPLSFQEFLEQLRRFRDQL 2501
(horse cathelicidin) PFP
AP00688 Ref, eCATH-3 KRFHSVGSLIQRHQQMIRDKSEAT 2502
(horse cathelicidin) RHGIRIITRPKLLLAS
AP00689 Ref, Prophenin-1 AFPPPNVPGPRFPPPNFPGPRFPPPN 2503
(pig cathelicidin) FPGPRFPPPNFPGPRFPPPNFPGPPFP
PPIFPGPWFPPPPPFRPPPFGPPRFP
AP00690 Ref, Prophenin-2 AFPPPNVPGPRFPPPNVPGPRFPPPN 2504
(pig cathelicidin) FPGPRFPPPNFPGPRFPPPNFPGPPFP
PPIFPGPWFPPPPPFRPPPFGPPRFP
AP00691 Ref, HFIAP-1 GFFKKAWRKVKHAGRRVLDTAK 2505
(hagfish GVGRHYVNNWLNRYR
cathelicidin)
AP00692 Ref, HFIAP-3 GWFKKAWRKVKNAGRRVLKGVG 2506
(hagfish IHYGVGLI
cathelicidin)
AP00693 Ref, Trout cath RICSRDKNCVSRPGVGSIIGRPGGG 2507
(fish cathelicidin) SLIGRPGGGSVIGRPGGGSPPGGGS
FNDEFIRDHSDGNRFA
AP00694 Ref, MRP AIGSILGALAKGLPTLISWIKNR 2508
(melittin-related
peptide)
AP00695 Ref, Temporin- FLPILGKLLSGIL 2509
1TGa (frog)
AP00696 Ref, Dahlein 1.1 GLFDIIKNIVSTL 2510
(frog)
AP00697 Ref, Dahlein 1.2 GLFDIIKNIFSGL 2511
(frog)
AP00698 Ref, Dahlein 4.1 GLWQLIKDKIKDAATGFVTGIQS 2512
(frog)
AP00699 Ref, Dahlein 4.2 GLWQFIKDKLKDAATGLVTGIQS 2513
(frog)
AP00700 Ref, Dahlein 4.3 GLWQFIKDKFKDAATGLVTGIQS 2514
(frog)
AP00701 Ref, Dahlein 5.1 GLLGSIGNAIGAFIANKLKP 2515
(frog)
AP00702 Ref, Dahlein 5.2 GLLGSIGNAIGAFIANKLKPK 2516
(frog)
AP00703 Ref, Dahlein 5.3 GLLASLGKVLGGYLAEKLKP 2517
(frog)
AP00704 Ref, Dahlein 5.4 GLLGSIGKVLGGYLAEKLKPK 2518
(frog)
AP00705 Ref, Dahlein 5.5 GLLASLGKVLGGYLAEKLKPK 2519
(frog)
AP00706 Ref, Dahlein 5.6 GLLASLGKVFGGYLAEKLKPK 2520
(frog)
AP00709 Ref, Mytilus GFGCPNDYPCHRHCKSIPGRAGGY 2521
defensin (mytilin) CGGAHRLRCTCYR
A (mollusc)
AP00711 Ref, Mussel GFGCPNNYACHQHCKSIRGYCGG 2522
defensin MGD2 YCAGWFRLRCTCYRCG
AP00712 Ref, scorpion GFGCPLNQGACHRHCRSIRRRGGY 2523
defensin CAGFFKQTCCYRN
AP00713 Ref, Androctonus GFGCPFNQGACHRHCRSIRRRGGY 2524
defensin CAGLFKQTCTCYR
AP00714 Ref, Orinthodoros GYGCPFNQYQCHSHCSGIRGYKGG 2525
defensin A (soft YCKGTFKQTCKCY
ticks)
AP00715 Ref, VaD1 (plant RTCMKKEGWGKCLIDTTCAHSCK 2526
defensin) NRGYIGGNCKGMTRTCYCLVNC
AP00722 Ref, Cryptonin GLLNGLALRLGKRALKKIIKRLCR 2527
(insect, cicada)
AP00723 Ref, Decoralin SLLSLLRKLIT 2528
(insect)
AP00724 Ref, RTD-2 (rhesus RCLCRRGVCRCLCRRGVC 2529
theta-defensin-2,
minidefensin,
XXC, BBS, lectin,
ZZHa)
AP00725 Ref, RTD-3 (rhesus RCICTRGFCRCICTRGFC 2530
theta-defensin-3,
minidefensin,
XXC, BBS, lectin,
ZZHa)
AP00726 Ref, Combi-1 RRWWRF 2531
(synthetic)
AP00748 Ref, Gm pro-rich DIQIPGIKKPTHRDIIIPNWNPNVRT 2532
pept1 (insect) QPWQRFGGNKS
AP00749 Ref, Gm anionic EADEPLWLYKGDNIERAPTTADHP 2533
pept 1 (insect) ILPSIIDDVKLDPNRRYA
AP00750 Ref, Gm pro-rich EIRLPEPFRFPSPTVPKPIDIDPILPHP 2534
pept 2 (insect) WSPRQTYPIIARRS
AP00752 Ref, Gm defensin- DKLIGSCVWGATNYTSDCNAECK 2535
like peptide (insect) RRGYKGGHCGSFWNVNCWCEE
AP00753 Ref, Gm VQETQKLAKTVGANLEETNKKLA 2536
apolipophoricin PQIKSAYDDFVKQAQEVQKKLHE
(insect) AASKQ
AP00754 Ref, Gm anionic ETESTPDYLKNIQQQLEEYTKNFNT 2537
pept2 (insect) QVQNAFDSDKIKSEVNNFIESLGKI
LNTEKKEAPK
AP00755 Ref, Gm cecropin ENFFKEIERAGQRIRDAIISAAPAVE 2538
D-like pept, insect TLAQAQKIIKGGD
AP00756 Ref, Dermaseptin- ALWKDILKNAGKAALNEINQLVNQ 2539
B6 (DRS-B6, DRS
B6, XXA, frog)
AP00759 Ref, Phylloseptin- FLSLIPHAINAVSTLVHHSG 2540
O1 (PLS-O1,
Phylloseptin-4, PS-
4, XXA, frog)
AP00760 Ref, Phylloseptin- FLSLIPHAINAVSAIAKHS 2541
O2 (PLS-O2,
Phylloseptin-5, PS-
5, XXA, frog)
AP00761 Ref, Phylloseptin-6 SLIPHAINAVSAIAKHF 2542
(Phylloseptin-H4,
PLS-H4, PS-6,
XXA, frog)
AP00762 Ref, Phylloseptin-7 FLSLIPHAINAVSAIAKHF 2543
(Phylloseptin-H5,
PLS-H5, PS-7,
XXA, frog)
AP00763 Ref, Dermaseptin GLWSTIKNVGKEAAIAAGKAALG 2544
DPh-1 (XXA, frog) AL
AP00764 Ref, Dermaseptin- GLRSKIWLWVLLMIWQESNKFKKM 2545
S9 (DRS-S9, DRS
S9, frog)
AP00765 Ref, Human salvic MHDFWVLWVLLEYIYNSACSVLS 2546
ATSSVSSRVLNRSLQVKVVKITN
AP00766 Ref, Gassericin A IYWIADQFGIHLATGTARKLLDAM 2547
(XXC, XXD2, ASGASLGTAFAAILGVTLPAWALA
class IV AAGALGATAA
bacteriocin, Gram-
positive bacteria)
AP00767 Ref, Circularin A VAGALGVQTAAATTIVNVILNAGT 2548
(XXC, class IV LVTVLGIIASIASGGAGTLMTIGWA
bacteriocin, Gram- TFKATVQKLAKQSMARAIAY
positive bacteria)
AP00768 Ref, Closticin 574 PNWTKIGKCAGSIAWAIGSGLFGG 2549
(bacteria) AKLIKIKKYIAELGGLQKAAKLLV
GATTWEEKLHAGGYALINLAAELT
GVAGIQANCF
AP00769 Ref, Caerin 1.11 GLLGAMFKVASKVLPHVVPAITEHF 2550
(XXA, frog)
AP00770 Ref, Maculatin 1.4 GLLGLLGSVVSHVLPAITQHL 2551
(XXA, frog)
AP00771 Ref, Magainin 1 GIGKFLHSAGKFGKAFVGEIMKS 2552
(frog)
AP00772 Ref, Oxyopinin 1 FRGLAKLLKIGLKSFARVLKKVLP 2553
(spider) KAAKAGKALAKSMADENAIRQQNQ
AP00773 Ref, Oxyopinin 2a GKFSVFGKILRSIAKVFKGVGKVR 2554
(spider) KQFKTASDLDKNQ
AP00774 Ref, Oxyopinin 2b GKFSGFAKILKSIAKFFKGVGKVR 2555
(spider) KGFKEASDLDKNQ
AP00775 Ref, Oxyopinin 2c GKLSGISKVLRAIAKFFKGVGKAR 2556
(spider) KQFKEASDLDKNQ
AP00776 Ref, Oxyopinin 2d GKFSVFSKILRSIAKVFKGVGKVRK 2557
(spider) GFKTASDLDKNQ
AP00777 Ref, NRC-1 (XXA, GKGRWLERIGKAGGIIIGGALDHL 2558
fish, gene
predicted)
AP00778 Ref, NRC-2 (XXA, WLRRIGKGVKIIGGAALDHL 2559
fish, gene
predicted)
AP00779 Ref, NRC-3 (XXA, GRRKRKWLRRIGKGVKIIGGAALD 2560
fish, gene HL
predicted)
AP00781 Ref, NRC-5 (XXA, FLGALIKGAIHGGRFIHGMIQNHH 2561
fish, gene
predicted)
AP00782 Ref, NRC-6 (XXA, GWGSIFKHGRHAAKHIGHAAVNH 2562
fish, gene YL
predicted)
AP00783 Ref, NRC-7 (XXA, RWGKWFKKATHVGKHVGKAALT 2563
fish, gene AYL
predicted)
AP00784 Ref, NRC-10 FFRLLFHGVHHVGKIKPRA 2564
(XXA, fish, gene
predicted)
AP00785 Ref, NRC-11 GWKSVFRKAKKVGKTVGGLALD 2565
(XXA, fish, gene HYL
predicted)
AP00786 Ref, NRC-12 GWKKWFNRAKKVGKTVGGLAVD 2566
(XXA, fish, gene HYL
predicted)
AP00787 Ref, NRC-13 GWRLLLKKAEVKTVGKLALKHYL 2567
(XXA, fish, gene
predicted)
AP00788 Ref, NRC-14 AGWGSIFKHIFKAGKFIHGAIQAHND 2568
(XXA, fish, gene
predicted)
AP00789 Ref, NRC-15 GFWGKLFKLGLHGIGLLHLHL 2569
(XXA, fish, gene
predicted)
AP00790 Ref, NRC-16 GWKKWLRKGAKHLGQAAIK 2570
(XXA, fish, gene
predicted)
AP00791 Ref, NRC-17 GWKKWLRKGAKHLGQAAIKGLAS 2571
(XXA, fish, gene
predicted)
AP00792 Ref, NRC-19 FLGLLFHGVHHVGKWIHGLIHGHH 2572
(XXA, fish, gene
predicted)
AP00793 Ref, Bombinin H2 IIGPVLGLVGSALGGLLKKI 2573
(XXA, frog)
AP00794 Ref, Bombinin H3 IIGPVLGMVGSALGGLLKKI 2574
(frog, XXD, XXA)
AP00795 Ref, Bombinin H7 ILGPILGLVSNALGGLL 2575
(frog, XXD, XXA)
AP00796 Ref, Bombinin GH- IIGPVLGLVGKPLESLLE 2576
1L (XXA, toad)
AP00797 Ref, Bombinin GH- IIGPVLGLVGKPLESLLE 2577
1D (toad, XXD,
XXA)
AP00807 Ref, Enterocin E- NRWYCNSAAGGVGGAAGCVLAG 2578
760 (bacteriocin, YVGEAKENIAGEVRKGWGMAGGF
bacteria) THNKACKSFPGSGWASG
AP00808 Ref, hepcidin (fish) CRFCCRCCPRMRGCGLCCRF 2579
AP00809 Ref, hepcidin TH1- GIKCRFCCGCCTPGICGVCCRF 2580
5 (fish)
AP00810 Ref, hepcidin TH2- QSHLSLCRWCCNCCRSNKGC 2581
3 (fish)
AP00811 Ref, human LEAP-2 MTPFWRGVSLRPIGASCRDDSECIT 2582
RLCRKRRCSLSVAQE
AP00812 Ref, Enkelytin FAEPLPSEEEGESYSKEPPEMEKRY 2583
(cow) GGFM
AP00732 Ref, Spheniscin-1 SFGLCRLRRGSCAHGRCRFPSIPIG 2584
(Sphe-1, avian RCSRFVQCCRRVW
defensin)
AP00733 Ref, Organgutan LLGDFFRKAREKIGEEFKRIVQRIK 2585
ppyLL-37 (Great DFLRNLVPRTES
Ape, primate
cathelicidin)
AP00734 Ref, Gibbon SLGNFFRKARKKIGEEFKRIVQRIK 2586
hmdSL-37 DFLQHLIPRTEA
(hylobatidae,
primate
cathelicidin)
AP00735 Ref, pobRL-37 RLGNFFRKAKKKIGRGLKKIGQKI 2587
(cercopithecidae, KDFLGNLVPRTES
primate
cathelicidin)
AP00736 Ref, cjaRL-37 RLGDILQKAREKIEGGLKKLVQKI 2588
(primate KDFFGKFAPRTES
cathelicidin)
AP00737 Ref, Plasticin GLVTSLIKGAGKLLGGLFGSVTG 2589
PBN2KF (XXA,
DRP-PBN2, frog)
AP00738 Ref, Plasticin GLVTGLLKTAGKLLGDLFGSLTG 2590
ANCKF (XXA,
synthetic)
AP00739 Ref, Plasticin GVVTDLLKTAGKLLGNLFGSLSG 2591
PD36KF (XXA,
synthetic)
AP00740 Ref, Plasticin GVVTDLLKTAGKLLGNLVGSLSG 2592
PD36K (XXA,
synthetic)
AP00741 Ref, Chicken PITYLDAILAAVRLLNQRISGPCILR 2593
cathelicidin-B1 LREAQPRPGWVGTLQRRREVSFLV
(bird cathelicidin) EDGPCPPGVDCRSCEPGALQHCVG
TVSIEQQPTAELRCRPLRPQ
AP00742 Ref, Chicken MRILYLLLSVLFVVLQGVAGQPYF 2594
gallinacin 4 (Gal 4) SSPIHACRYQRGVCIPGPCRWPYY
RVGSCGSGLKSCCVRNRWA
AP00743 Ref, Chicken MKILCFFIVLFVAVHGAVGFSRSPR 2595
gallinacin 7 (Gal 7) YHMQCGYRGTFCTPGKCPYGNAY
LGLCRPKYSCCRWL
AP00744 Ref, Chicken MQILPLLFAVLLLMLRAEPGLSLA 2596
gallinacin 9 (Gal 9) RGLPQDCERRGGFCSHKSCPPGIGR
IGLCSKEDFCCRSRWYS
AP00745 Ref, Chicken MTPFWRGVSLRPVGASCRDNSECI 2597
LEAP-2 (cLEAP- TMLCRKNRCFLRTASE
2)
AP00814 Ref, Caerulein GLGSILGKILNVAGKVGKTIGKVA 2598
precursor-related DAVGNKE
fragment Ea
(CPRF-Ea, frog)
AP00815 Ref, Caerulein GLGSFLKNAIKIAGKVGSTIGKVAD 2599
precursor-related AIGNKE
fragment Eb
(CPRF-Eb, frog)
AP00816 Ref, Caerulein GLGSFFKNAIKIAGKVGSTIGKVAD 2600
precursor-related AIGNKE
fragment Ec
(CPRF-Ec, frog)
AP00817 Ref, Temporin-1Oa FLPLLASLFSRLL 2601
(frog)
AP00818 Ref, Temporin-1Ob FLPLIGKILGTIL 2602
(frog)
AP00819 Ref, Temporin-1Oc FLPLLASLFSRLF 2603
(frog)
AP00820 Ref, Temporin-1Od FLPLLASLFSGLF 2604
(frog)
AP00821 Ref, Brevinin-20a GLFNVFKGLKTAGKHVAGSLLNQ 2605
(frog) LKCKVSGGC
AP00822 Ref, Brevinin-20b GIFNVFKGALKTAGKHVAGSLLNQ 2606
(frog) LKCKVSGEC
AP00824 Ref, Temporin-1Gb SILPTIVSFLSKFL 2607
(XXA, frog)
AP00825 Ref, Temporin-1Gc SILPTIVSFLTKFL 2608
(XXA, frog)
AP00826 Ref, Temporin-1Gd FILPLIASFLSKFL 2609
(XXA, frog)
AP00827 Ref, Ranatuerin- SMISVLKNLGKVGLGFVACKVNK 2610
1Ga (frog) QC
AP00829 Ref, Ranalexin-1G FLGGLMKIIPAAFCAVTKKC 2611
(frog)
AP00830 Ref, Ranatuerin-2G GLLLDTLKGAAKDIAGIALEKLKC 2612
(frog) KITGCKP
AP00831 Ref, Odorranain- GLLSGILGAGKHIVCGLTGCAKA 2613
NR (frog)
AP00832 Ref, Maximin H1 ILGPVISTIGGVLGGLLKNL 2614
(XXA, toad)
AP00834 Ref, G. mellonella KVNANAIKKGGKAIGKGFKVISAA 2615
moricin-like STAHDVYEHIKNRRH
peptide A (Gm-
mlpA, insect)
AP00835 Ref, G. mellonella GKIPVKAIKKGGQIIGKALRGINIAS 2616
moricin-like TAHDIISQFKPKKKKNH
peptide B (Gm-
mlpB, insect)
AP00836 Ref, G. mellonella KVPIGAIKKGGKIIKKGLGVIGAAG 2617
moricin-like TAHEVYSHVKNRH
peptide C1 (Gm-
mlpC1, insect)
AP00837 Ref, G. mellonella KVPIGAIKKGGKIIKKGLGVLGAA 2618
moricin-like GTAHEVYNHVRNRQ
peptide C2 (Gm-
mlpC2, insect)
AP00838 Ref, G. mellonella KVPIGAIKKGGKIIKKGLGVIGAAG 2619
moricin-like TAHEVYSHVKNRQ
peptide C3 (Gm-
mlpC3, insect)
AP00839 Ref, G. mellonella KVPVGAIKKGGKAIKTGLGVVGA 2620
moricin-like AGTAHEVYSHIRNRH
peptide C4/C5
(Gm-mlpC4/C5,
insect)
AP00840 Ref, G. mellonella KGIGSALKKGGKIIKGGLGALGAIG 2621
moricin-like TGQQVYEHVQNRQ
peptide D (Gm-
mlpD, insect)
AP00841 Ref, Enterocin A TTHSGKYYGNGVYCTKNKCTVD 2622
(EntA, class IIA WAKATTCIAGMSIGGFLGGAIPGKC
bacteriocin, i.e.
pediocin-like
peptide, bacteria)
AP00842 Ref, Divercin V41 TKYYGNGVYCNSKKCWVDWGQA 2623
(DvnV41, class IIa SGCIGQTVVGGWLGGAIPGKC
bacteriocin,
pediocin-like
peptide, bacteria.
DvnRV41 is the
recombinant form)
AP00843 Ref, Divergicin TKYYGNGVYCNSKKCWVDWGTA 2624
M35 (class IIa QGCIDVVIGQLGGGIPGKGKC
bacteriocin,
pediocin-like
peptide, bacteria)
AP00844 Ref, Coagulin KYYGNGVTCGKHSCSVDWGKATT 2625
(bacteriocin, CIINNGAMAWATGGHQGTHKC
pediocin-like
peptide, bacteria)
AP00845 Ref, Listeriocin KSYGNGVHCNKKKCWVDWGSAIS 2626
743A (class IIa TIGNNSAANWATGGAAGWKS
bacteriocin,
pediocin-like
peptide, bacteria)
AP00846 Ref, Mundticin KS KYYGNGVSCNKKGCSVDWGKAIG 2627
(enterocin CRL35, IIGNNSAANLATGGAAGWKS
mundticin ATO6,
mundticin QU2,
class IIa
bacteriocin,
pediocin-like
peptide, bacteria)
AP00847 Ref, Sakacin 5X KYYGNGLSCNKSGCSVDWSKAISII 2628
(Sak5X, class IIa GNNAVANLTTGGAAGWKS
bacteriocin,
pediocin-like
peptide, bacteria)
AP00848 Ref, Leucocin C KNYGNGVHCTKKGCSVDWGYAW 2629
(class IIa ANIANNSVMNGLTGGNAGWHN
bacteriocin,
pediocin-like
peptide, bacteria)
AP00849 Ref, Lactococcin TSYGNGVHCNKSKCWIDVSELETY 2630
MMFII (class IIa KAGTVSNPKDILW
bacteriocin,
pediocin-like
peptide, bacteria)
AP00850 Ref, Sakacin G KYYGNGVSCNSHGCSVNWGQAW 2631
(SakG, class IIa TCGVNHLANGGHGVC
bacteriocin,
pediocin-like
peptide, bacteria)
AP00851 Ref, Plantaricin KYYGNGVTCGKHSCSVNWGQAFS 2632
423 (class IIa CSVSHLANFGHGKC
bacteriocin,
pediocin-like
peptide, bacteria)
AP00852 Ref, Plantaricin KYYGNGLSCSKKGCTVNWGQAFS 2633
C19 (class IIa CGVNRVATAGHHKC
bacteriocin,
pediocin-like
peptide, bacteria)
AP00853 Ref, Enterocin P ATRSYGNGVYCNNSKCWVNWGE 2634
(EntP, class IIa AKENIAGIVISGWASGLAGMGH
bacteriocin,
pediocin-like
peptide, bacteria)
AP00854 Ref, Bacteriocin 31 ATYYGNGLYCNKQKCWVDWNKA 2635
(Bac 31, Bac31, SREIGKIIVNGWVQHGPWAPR
class IIa
bacteriocin,
pediocin-like
peptide, bacteria)
AP00855 Ref, MSI-78 GIGKFLKKAKKFGKAFVKILKK 2636
(XXA, synthetic)
AP00856 Ref, MSI-594 GIGKFLKKAKKGIGAVLKVLTTGL 2637
(XXA, synthetic)
AP00857 Ref, Catestatin SSMKLSFRARAYGFRGPGPQL 2638
(human
CHGA(352-372),
human Cst)
AP00858 Ref, Temporin D LLPIVGNLLNSLL 2639
(XXA, frog)
AP00859 Ref, Temporin H LSPNLLKSLL 2640
(XXA, frog)
AP00861 Ref, Brevinin-ALb FLPLAVSLAANFLPKLFCKITKKC 2641
(frog)
AP00862 Ref, Brevinin 1E FLPLLAGLAANFLPKIFCKITKRC 2642
(frog)
AP00863 Ref, Temporin- FLPIVGKLLSGLSGLL 2643
ALa (XXA, frog)
AP00864 Ref, Temporin FLPIVGRLISGLL 2644
1ARa (XXA, frog)
AP00865 Ref, Temporin FLPIIGQLLSGLL 2645
1AUa (XXA,
Temporin-1AUa)
(frog)
AP00866 Ref, Temporin FLPIIAKVLSGLL 2646
1Bya (XXA,
Temporin-1Bya,
frog)
AP00867 Ref, Temporin 1Ec FLPVIAGLLSKLF 2647
(XXA, frog)
AP00869 Ref, Temporin 1Ja ILPLVGNLLNDLL 2648
(XXA, Temporin-
1Ja, frog)
AP00873 Ref, Temporin 1Pra ILPILGNLLNGLL 2649
(XXA, frog)
AP00874 Ref, Temporin 1VE FLPLVGKILSGLI 2650
(XXA, frog)
AP00875 Ref, Temporin 1Va FLSSIGKILGNLL 2651
(XXA, frog)
AP00876 Ref, Temporin 1Vb FLSIIAKVLGSLF 2652
(XXA, frog)
AP00877 Ref, Brevinin-1Ja FLGSLIGAAIPAIKQLLGLKK 2653
(frog)
AP00878 Ref, Brevinin- FLPILASLAAKFGPKLFCLVTKKC 2654
1BYa (frog)
AP00884 Ref, Ixosin-B (tick) QLKVDLWGTRSGIQPEQHSSGKSD 2655
VRRWRSRY
AP00885 Ref, Brevinin- FLPILASLAAKLGPKLFCLVTKKC 2656
1BYb (frog)
AP00886 Ref, Brevinin- FLPILASLAATLGPKLLCLITKKC 2657
1BYc (frog)
AP00887 Ref, Brevinin- GILSTFKGLAKGVAKDLAGNLLDK 2658
2BYa (frog) FKCKITGC
AP00888 Ref, Brevinin- GIMDSVKGLAKNLAGKLLDSLKC 2659
2BYb (frog) KITGC
AP00891 Ref, Pilosulin 3 IIGLVSKGTCVLVKTVCKKVLKQG 2660
(Myr b III)(ants)
AP00892 Ref, Pilosulin 4 PDITKLNIKKLTKATCKVISKGASM 2661
(Myr b IV)(ants) CKVLFDKKKQE
AP00893 Ref, Pilosulin 5 DVKGMKKAIKGILDCVIEKGYDKL 2662
(Myr b III)(ants) AAKLKKVIQQLWE
AP00894 Ref, Ocellatin 4 GLLDFVTGVGKDIFAQLIKQI 2663
(XXA, frog)
AP00895 Ref, OH-CATH KRFKKFFKKLKNSVKKRAKKFFK 2664
(snake cathelicidin, KPRVIGVSIPF
reptile cathelicidin,
or elapid
cathelicidins)
AP00896 Ref, BF-CATH KRFKKFFKKLKKSVKKRAKKFFK 2665
(snake cathelicidin) KPRVIGVSIPF
AP00897 Ref, NA-CATH KRFKKFFKKLKNSVKKRAKKFFK 2666
(snake cathelicidin) KPKVIGVTFPF
AP00898 Ref, Temporin-1Sa FLSGIVGMLGKLF 2667
(XXA, frog)
AP00899 Ref, Temporin-1Sb FLPIVTNLLSGLL 2668
(XXA, frog)
AP00900 Ref, Temporin-1Sc FLSHIAGFLSNLF 2669
(XXA, frog)
AP00913 Ref, Ib-AMP1 EWGRRCCGWGPGRRYCVRWC 2670
(IbAMP1, plant
defensin)
AP00914 Ref, Ib-AMP2 QYGRRCCNWGPGRRYCKRWC 2671
(IBAMP2, plant
defensin)
AP00915 Ref, Ee-CBP QQCGRQAGNRRCANNLCCSQYGY 2672
(EeCBP, plant CGRTNEYCCTSQGCQSQCRRCG
defensin, hevein-
type, E. europaeus
chitin-binding
protein)
AP00916 Ref, Pa-AMP1 AGCIKNGGRCNASAGPPYCCSSYC 2673
(PaAMP1, plant FQIAGQSYGVCKNR
defensin, C6 type)
AP00917 Ref, Pa-AMP2 ACIKNGGRCVASGGPPYCCSNYCL 2674
(PaAMP2, plant QIAGQSYGVCKKH
defensin, C6 type)
AP00924 Ref, Ornithodoros GYGCPFNQYQCHSHCRGIRGYKG 2675
defensin B (soft GYCTGRFKQTCKCY
ticks)
AP00925 Ref, Ornithodoros GYGCPFNQYQCHSHCSGIRGYKGG 2676
defensin C (soft YCKGLFKQTCNCY
ticks)
AP00926 Ref, Ornithodoros GFGCPFNQYECHAHCSGVPGYKG 2677
defensin D (soft GYCKGLFKQTCNCY
ticks)
AP00927 Ref, IYFIADKMGIQLAPAWYQDIVNWV 2678
Butyrivibriocin SAGGTLTTGFAIIVGVTVPAWIAEA
AR10 (XXC, class AAAFGIASA
IV bacteriocin,
gram-positive
bacteria)
AP00929 Ref, AS-48 ASLQFLPIAHMAKEFGIPAAVAGT 2679
(enterocin 4, XXC, VINVVEAGGWVTTIVSILTAVGSG
class IV bacteriocin GLSLLAAAGRESIKAYLKKEIKKK
or class IId GKRAVIAW
bacteriocin, Gram-
positive bacteria)
AP00930 Ref, Reutericin 6 IYWIADQFGIHLATGTARKLLDAM 2680
(XXC, XXD1, ASGASLGTAFAAILGVTLPAWALA
class IV AAGALGATAA
bacteriocin, Gram-
positive bacteria)
AP00931 Ref, Uberolysin LAGYTGIASGTAKKVVDAIDKGAA 2681
(XXC, class IV AFVIISIISTVISAGALGAVSASADFI
bacteriocin, Gram- ILTVKNYISRNLKAQAVIW
positive bacteria)
AP00932 Ref, Acidocin B IYWIADQFGIHLATGTARKLLDAV 2682
(XXC, class IV ASGASLGTAFAAILGVTLPAWALA
bacteriocin, Gram- AAGALGATAA
positive bacteria)
AP00980 Ref, Phormia ATCDLLSGTGINHSACAAHCLLRG 2683
defensin B (insect NRGGYCNRKGVCVCRN
defensin B)
AP00990 Ref, Pth-St1 (plant RNCESLSHRFKGPCTRDSN 2684
defensin)
AP00991 Ref, Snakin-1 GSNFCDSKCKLRCSKAGLADRCLK 2685
(StSN1, plant YCGICCEECKCVPSGTYGNKHECP
defensin) CYRDKKNSKGKSKCP
AP00992 Ref, Snakin-2 YSYKKIDCGGACAARCRLSSRPRL 2686
(StSN2, plant CNRACGTCCARCNCVPPGTSGNTE
defensin) TCPCYASLTTHGNKRKCP
AP00993 Ref, So-D2 (S. oleracea GIFSSRKCKTPSKTFKGICTRDSNC 2687
defensin DTSCRYEGYPAGDCKGIRRRCMCS
D2, plant defensin) KPC
AP00994 Ref, So-D6 (S. oleracea GIFSNMYARTPAGYFRGP 2688
defensin
D6, plant defensin)
AP00997 Ref, Nisin Q ITSISLCTPGCKTGVLMGCNLKTAT 2689
(lantibiotic, CNCSVHVSK
bacteriocins,
bacteria)
AP01008 Ref, Tachystatin YSRCQLQGFNCVVRSYGLPTIPCC 2690
A1 (BBS, RGLTCRSYFPGSTYGRCQRF
horseshoe crabs)
AP01009 Ref, Tachystatin C DYDWSLRGPPKCATYGQKCRTWS 2691
(BBS, horseshoe PRNCCWNLRCKAFRCRPR
crabs)
AP01012 Ref, Latarcin 3a SWKSMAKKLKEYMEKLKQRA 2692
(Ltc3a, XXA,
BBM, spider)
AP01013 Ref, Latarcin 3b SWASMAKKLKEYMEKLKQRA 2693
(Ltc3b, XXA,
BBM, spider)
AP01014 Ref, Latarcin 4a GLKDKFKSMGEKLKQYIQTWKAKF 2694
(Ltc4a, XXA,
BBM, spider)
AP01015 Ref, Latarcin 4b SLKDKVKSMGEKLKQYIQTWKAKF 2695
(Ltc4b, XXA,
BBM, spider)
AP01016 Ref, Latarcin 5 GFFGKMKEYFKKFGASFKRRFANL 2696
(Ltc5, XXA, BBM, KKRL
spider)
AP01018 Ref, Latarcin 6a QAFQTFKPDWNKIRYDAMKMQTS 2697
(Ltc6a, BBM, LGQMKKRFNL
spider)
AP01019 Ref, Latarcin 7 GETFDKLKEKLKTFYQKLVEKAED 2698
(Ltc7, BBM, LKGDLKAKLS
spider)
AP01049 Ref, Kalata B2 VCGETCFGGTCNTPGCSCTWPICT 2699
(plant cyclotides, RDGLP
XXC)
AP01141 Ref, Cryptdin-6 LRDLVCYCRARGCKGRERMNGTC 2700
(Crp6, animal RKGHLLYMLCCR
defensin, alpha,
mouse)
AP01142 Ref, Rabbit kidney KPYCSCKWRCGIGEEEKGICHKFPI 2701
defensin RK-2 VTYVCCRRP
(animal defensin,
alpha-defensin)
AP01146 Ref, Gallinacin 6 DTLACRQSHGSCSFVACRAPSVDI 2702
(Gal6, Gal-6, avian GTCRGGKLKCCKWAPSS
beta defensin, bird)
AP01147 Ref, Gallinacin 8 DTVACRIQGNFCRAGACPPTFTISG 2703
(Gal8, Gal-8, avian QCHGGLLNCCAKIPAQ
beta defensin, bird)
AP01148 Ref, Gallinacin 3 IATQCRIRGGFCRVGSCRFPHIAIGK 2704
(Gal3, Gal-3, avian CATFISCCGRAY
beta defensin, bird)
AP01152 Ref, Lactococcin Q SIWGDIGQGVGKAAYWVGKAMG 2705
(class IIb NMSDVNQASRINRKKKH
bacteriocin,
bacteria, chain a.
For chain b, see
Info)
AP01155 Ref, Enterocin ESVFSKIGNAVGPAAYWILKGLGN 2706
1071 (Ent1071A, MSDVNQADRINRKKH
class IIb
bacteriocin,
bacteria; chain B is
Enterocin 1071B or
Ent1071B, see
info)
AP01156 Ref, Plantaricin S NKLAYNMGHYAGKATIFGLAAW 2707
(chain a, class IIb ALLA
bacteriocin,
bacteria)
AP01159 Ref, Hinnavin II KWKIFKKIEHMGQNIRDGLIKAGP 2708
(Hin II, XXA, AVQVVGQAATIYK
insect)
AP01160 Ref, NK-2 KILRGLCKKIMRSFLRRISWDILTG 2709
(synthetic, XXA) KK
AP01167 Ref, Plantaricin LTTKLWSSWGYYLGKKARWNLK 2710
NC8 (PLNC8, HPYVQF
chain a, class IIb
bacteriocin,
bacteria. For chain
b, see Info)
AP01168 Ref, Carnocyclin A LVAYGIAQGTAEKVVSLINAGLTV 2711
(a circular GSIISILGGVTVGLSGVFTAVKAAI
bacteriocin, XXC, AKQGIKKAIQL
bacteria)
AP01169 Ref, Lactacin F NRWGDTVLSAASGAGTGIKACKSF 2712
(LafX, class IIb GPWGMAICGVGGAAIGGYFGYTHN
bacteriocin,
bacteria. For LafA,
see Info)
AP01170 Ref, Brochocin C YSSKDCLKDIGKGIGAGTVAGAAG 2713
(BrcC, chain BrcA, GGLAAGLGAIPGAFVGAHFGVIGG
class IIb SAACIGGLLGN
bacteriocin,
bacteria. For BrcB,
see Info)
AP01171 Ref, Thermophilin YSGKDCLKDMGGYALAGAGSGAL 2714
13 (chain a ThmA, WGAPAGGVGALPGAFVGAHVGAI
2-chain class IIb AGGFACMGGMIGNKFN
bacteriocin,
bacteria. For chain
B ThmB, see Info)
AP01172 Ref, ABP-118 KRGPNCVGNFLGGLFAGAAAGVP 2715
(chain a: LGPAGIVGGANLGMVGGALTCL
Abp118alpha, class
IIb bacteriocin,
bacteria. For chain
b: Abp118beta, see
Info)
AP01173 Ref, Salivaricin P KRGPNCVGNFLGGLFAGAAAGVP 2716
(chain a: Sln1; LGPAGIVGGANLGMVGGALTCL
class IIb
bacteriocin,
bacteria. For chain
b: Sln2, see Info)
AP01174 Ref, Mutacin IV KVSGGEAVAAIGICATASAAIGGL 2717
(chain a: NlmA, AGATLVTPYCVGTWGLIRSH
class IIb
bacteriocin,
bacteria. For chain
b: NLmB, see Info)
AP01175 Ref, Lactocin 705 GMSGYIQGIPDFLKGYLHGISAAN 2718
(chain a: KHKKGRLGY
Lac705alpha; class
IIb bacteriocin,
bacteria. For chain
b: Lac705beta, see
Info)
AP01176 Ref, Cytolysin TTPACFTIGLGVGALFSAKFC 2719
(CylLS, bacteria;
Chain B: CylLL)
AP01177 Ref, Plantaricin EF FNRGGYNFGKSVRHVVDAIGSVA 2720
(chain a. PlnE, GILKSIR
class IIb
bacteriocin,
bacteria. Chain b:
PlnF)
AP01178 Ref, Plantaricin JK GAWKNFWSSLRKGFYDGEAGRAI 2721
(chain a: PlnJ; class RR
IIb bacteriocin,
bacteria. Chain b:
PlnK)
AP01179 Ref, Enterocin SE- NGVYCNKQKCWVDWSRARSEIID 2722
K4 (class IIa RGVKAYVNGFTKVLGGIGGR
bacteriocin,
bacteria)
AP01180 Ref, Acidocin NPKVAHCASQIGRSTAWGAVSGA 2723
J1132 (class IIb
bacteriocin,
bacteria)
AP01181 Ref, Curvaticin AYPGNGVHCGKYSCTVDKQTAIG 2724
L442 (class IIa NIGNNAA
bacteriocin,
bacteria)
AP01182 Ref, Bacteriocin 32 FTPSVSFSQNGGVVEAAAQRGYIY 2725
(Bac 32, class IIa KKYPKGAKVPNKVKMLVNIRGKQ
bacteriocin, TMRTCYLMSWTASSRTAKYYYYI
bacteria)
AP01183 Ref, Bacteriocin 43 ATYYGNGLYCNKEKCWVDWNQA 2726
(Bac 43, KGEIGKIIVNGWVNHGPWAPRR
bacteriocin,
bacteria)
AP01184 Ref, Bacteriocin T8 ATYYGNGLYCNKEKCWVDWNQA 2727
(Bac T8, class IIa KGEIGKIIVNGWVNHGPWAPRR
bacteriocin,
bacteria)
AP01185 Ref, Enterocin B ENDHRMPNNLNRPNNLSKGGAKC 2728
(EntB, bacteriocin, GAAIAGGLFGIPKGPLAWAAGLAN
bacteria) VYSKCN
AP01186 Ref, Acidocin A KTYYGTNGVHCTKKSLWGKVRLK 2729
(bacteriocin, NVIPGTLCRKQSLPIKQDLKILLGW
bacteria) ATGAFGKTFH
AP01187 Ref, Enterocin Q MNFLKNGIAKWMTGAELQAYKK 2730
(EntQ, class IIc KYGCLPWEKISC
bacteriocin,
leaderless, i.e. no
signal peptide,
bacteria)
AP01188 Ref, Enterocin MLAKIKAMIKKFPNPYTLAAKLTT 2731
EJ97 (EntEJ97, YEINWYKQQYGRYPWERPVA
class IIc
bacteriocin,
leaderless, i.e. no
signal peptide,
bacteria)
AP01189 Ref, Enterocin RJ- APAGLVAKFGRPIVKKYYKQIMQF 2732
11 (EntRJ-11, class IGEGSAINKIIPWIARMWRT
IIc bacteriocin,
leaderless, i.e. no
signal sequence,
bacteria)
AP01190 Ref, Enterocin L50 MGAIAKLVAKFGWPIVKKYYKQI 2733
(old name: MQFIGEGWAINKIIEWIKKHI
pediocin L50,
EntL50A, a two-
chain class IIc
bacteriocin,
leaderless, i.e. no
signal peptide,
bacteria. The
sequence of
EntL50B is
provided in Info)
AP01191 Ref, MR10 MGAIAKLVAKFGWPIVKKYYKQI 2734
(MR10A, class IIc MQFIGEGWAINKIIDWIKKHI
bacteriocin,
leaderless, i.e. no
signal peptide,
bacteria. For the
sequence of chain
b, see Info)
AP01192 Ref, Halocin S8 SDCNINSNTAADVILCFNQVGSCA 2735
(HalS8, LCSPTLVGGPVP
microhalocin,
archaeocins,
archeae)
AP01193 Ref, Halocin C8 DIDITGCSACKYAAGQVCTIGCSA 2736
(HalC8, AGGFICGLLGITIPVAGLSCLGFVEI
microhalocins, VCTVADEYSGCGDAVAKEACNRA
archaeocins, GLC
archaea)
AP01194 Ref, Lacticin 3147 CSTNTFSLSDYWGNNGAWCTLTH 2737
(chain A1, a two- ECMAWCK
chain lantibiotic,
bacteriocin,
bacteria. The
sequence of chain
A2 is given in Info;
XXD3)
AP01195 Ref, Salivaricin A KRGSGWIATITDDCPNSVFVCC 2738
(SalA, lantibiotic,
bacteriocin,
bacteria)
AP01196 Ref, Microcin E492 ATYYGNGLYCNKEKCWVDWNQA 2739
(MccE492, class KGEIGKIIVNGWVNHGPWAPRR
IIb microcins,
bacteriocin,
bacteria; BBM; u-
MccE492,
siderophore
peptide, BBI, XXG)
AP01197 Ref, Hiracin JM79 ATYYGNGLYCNKEKCWVDWNQA 2740
(HirJM79, a Sec- KGEIGKIIVNGWVNHGPWAPRR
dependent class II
bacteriocin,
bacteria)
AP01198 Ref, Thermophilin LSCDEGMLAVGGLGAVGGPWGA 2741
9 (BlpDst, class IIb AVGVLVGAALYCF
bacteriocin,
bacteria. beta-
chains: BlpUst,
BlpEst, BapFst)
AP01199 Ref, Penocin A KYYGNGVHCGKKTCYVDWGQAT 2742
(PenA, class IIa ASIGKIIVNGWTQHGPWAHR
bacteriocin,
bacteria)
AP01200 Ref, Salivaricin B GGGVIQTISHECRMNSWQFLFTCCS 2743
(SalB, lantibotic,
bacteriocin,
bacteria)
AP01201 Ref, Lacticin 481 KGGSGVIHTISHECNMNSWQFVFT 2744
(lantibiotic, class I CCS
bacteriocin,
bacteria)
AP01202 Ref, Bacteriocin KGGSGVIHTISHEVIYNSWNFVFTC 2745
J46 (BacJ46, CS
bacteriocin,
bacteria)
AP01203 Ref, Nukacin A KKKSGVIPTVSHDCHMNSFQFVFT 2746
(NucA, Nukacin CCS
ISK-1, NukISK-1,
bacteriocin,
bacteria)
AP01204 Ref, Streptococcin GKNGVFKTISHECHLNTWAFLATC 2747
A-FF22 CS
(LANTIBIOTIC,
class I bacteriocin,
bacteria)
AP01210 Ref, Jelleine-I PFKLSLHL 2748
(honeybees, insect,
XXA)
AP01211 Ref, Jelleine-II TPFKLSLHL 2749
(honeybees, insect,
XXA)
AP01212 Ref, Jelleine-III EPFKLSLHL 2750
(honeybees, insect,
XXA)
AP01213 Ref, EFRGSIVIQGTKEGKSRPSLDIDYK 2751
Hymenoptaecin QRVYDKNGMTGDAYGGLNIRPGQ
(honeybees, insect PSRQHAGFEFGKEYKNGFIKGQSE
defensin, XXcooh) VQRGPGGRLSPYFGINGGFRF
AP01216 Ref, Ascaphin-1 GFRDVLKGAAKAFVKTVAGHIAN 2752
(frog, XXA)
AP01218 Ref, Ascaphin-3 GFRDVLKGAAKAFVKTVAGHIANI 2753
(frog)
AP01220 Ref, Ascaphin-5 GIKDWIKGAAKKLIKTVASNIANQ 2754
(frog)
AP01222 Ref, Ascaphin-7 GFKDWIKGAAKKLIKTVASSIANQ 2755
(frog)
AP01223 Ref, Ascaphin-8 GFKDLLKGAAKALVKTVLF 2756
(frog, XXA)
AP01226 Ref, Microcin C7 MRTGNAD 2757
(MccC7, microcin
C51, MccC51,
class I microcins,
bacteriocins,
bacteria. Others:
MccA; XXamp;
BBPe)
AP01227 Ref, Microcin B17 VGIGGGGGGGGGGSCGGQGGGCG 2758
(MccB17, class I GCSNGCSGGNGGSGGSGSHI
microcins,
bacteriocins, Gram-
negative bacteria;
BBPe)
AP01228 Ref, Microcin V ASGRDIAMAIGTLSGQFVAGGIGA 2759
(MccV, (old name) AAGGVAGGAIYDYASTHKPNPAM
Colicin V, ColV; SPSGLGGTIKQKPEGIPSEAWNYAA
class II microcins, GRLCNWSPNNLSDVCL
bacteriocins, Gram-
negative bacteria)
AP01229 Ref, Microcin L GDVNWVDVGKTVATNGAGVIGG 2760
(MccL, class IIa AFGAGLCGPVCAGAFAVGSSAAV
microcins, AALYDAAGNSNSAKQKPEGLPPEA
bacteriocins, Gram- WNYAEGRMCNWSPNNLSDVCL
negative bacteria)
AP01230 Ref, Microcin M DGNDGQAELIAIGSLAGTFISPGFG 2761
(MccM, class IIb SIAGAYIGDKVHSWATTATVSPSM
microcins, SPSGIGLSSQFGSGRGTSSASSSAGS
bacteriocins, Gram- GS
negative bacteria)
AP01231 Ref, Microcin H47 GGAPATSANAAGAAAIVGALAGIP 2762
(MccH47, class IIb GGPLGVVVGAVSAGLTTGIGSTVG
microcins, SGSASSSAGGGS
bacteriocins, Gram-
negative bacteria)
AP01232 Ref, Microcin I47 MNLNGLPASTNVIDLRGKDMGTYI 2763
(MccI47, class IIb DANGACWAPDTPSIIMYPGGSGPS
microcins, YSMSSSTSSANSGS
bacteriocins, Gram-
negative bacteria)
Aibellin *Ac U A U A U A Q U F U G U U P V U U E E 2764
[NHC(CH2Ph)HCH2NHCH2CH2]OH
Alamethicin_F-30 *Ac U P U A U A Q U V U G L U P V U U E Q F 2765
OH
Alamethicin_F-50 * Ac U P U A U A Q U V U G L U P V U U Q Q F 2766
OH
Alamethicin_II * Ac U P U A U U Q U V U G L U P V U U E Q F 2767
OH
Ampullosporin * Ac W A U U L U Q U U U Q L U Q L OH 2768
Ampullosporin_B * Ac W A U U L U Q A U U Q L U Q L OH 2769
Ampullosporin_C * Ac W A U U L U Q U A U Q L U Q L OH 2770
Ampullosporin_D * Ac W A U U L U Q U U A Q L U Q L OH 2771
Ampullosporin_E1 * Ac W A U U L U Q A U U Q L A Q L OH 2772
Ampullosporin_E2 * Ac W A U U L U Q U A A Q L U Q L OH 2773
Ampullosporin_E3 * Ac W A U U L U Q U U A Q L A Q L OH 2774
Ampullosporin_E4 * Ac W A U U L U Q A A U Q L U Q L OH 2775
Antiamoebin_I * Ac F U U U J G L U U O Q J O U P F OH 2776
Antiamoebin_II * Ac F U U U J G L U U O Q J P U P F OH 2777
Antiamoebin_III * Ac F U U U U G L U U O Q J O U P F OH 2778
Antiamoebin_IV * Ac F U U U J G L U U O Q J O U P F OH 2779
Antiamoebin_V * Ac F U U U J A L U U O Q J O U P F OH 2780
Antiamoebin_VI * Ac F U U U U G L U U O Q U O U P F OH 2781
Antiamoebin_VII * Ac F A U J U G L U U O Q J O U P F OH 2782
Antiamoebin_VIII * Ac F U U U J G L U U O Q U O U P F OH 2783
Antiamoebin_IX * Ac F U A U J G L U U O Q J O U P F OH 2784
Antiamoebin_X * Ac F U U U J G L J U O Q U O U P F OH 2785
Antiamoebin_XI * Ac F U U U U A L U U O Q J O U P F OH 2786
Antiamoebin_XII * Ac F U U U U G L A U O Q J O U P F OH 2787
Antiamoebin_XIII * Ac V U U U U G L U U O Q J O U P F OH 2788
Antiamoebin_XIV * Ac V U U U V G L U U O Q J O U P F OH 2789
Antiamoebin_XV * Ac L U U U U G L U U O Q J O U P F OH 2790
Antiamoebin_XVI * Ac L U U U J G L U U O Q J O U P F OH 2791
Atroviridin_A * Ac U P U A U A Q U V U G L U P V U U Q Q F 2792
OH
Atroviridin_B * Ac U P U A U A Q U V U G L U P V U J Q Q F 2793
OH
Atroviridin_C * Ac U P U A U U Q U V U G L U P V U J Q Q F 2794
OH
Bergofungin_A * Ac V U U U V G L U U O Q J O U F OH 2795
Bergofungin_B * Ac V U U U V G L V U O Q U O U F OH 2796
Bergofungin_C * Ac V U U U V G L U U O Q U O U F OH 2797
Bergofungin_D * Ac V U U V G L U U O Q U O U F OH 2798
Boletusin * Ac F U A U J L Q G U U A A U P U U U Q W 2799
OH
Cephaibol_A * Ac F U U U U G L J U O Q J O U P F OH 2800
Cephaibol_A2 * Ac F U U U U A L J U O Q J O U P F OH 2801
Cephaibol_B * Ac F U U U J G L J U O Q J O U P F OH 2802
Cephaibol_C * Ac F U U U U G L J U O Q U O U P F OH 2803
Cephaibol_D * Ac F U U U U G L U U O Q U O U P F OH 2804
Cephaibol_E * Ac F U U U U G L U U O Q J O U P F OH 2805
Cephaibol_P * Ac F J Q U I T U L U O Q U O U P F S OH 2806
Cephaibol_Q * Ac F J Q U I T U L U P Q U O U P F S OH 2807
Cervinin_1 * Ac L U P U L U P A U P V L OH 2808
Cervinin_2 * Ac L U P U L U P A U P V L OCOCH3 2809
Chrysospermin_A * Ac F U S U U L Q G U U A A U P U U U Q W 2810
OH
Chrysospermin_B * Ac F U S U U L Q G U U A A U P J U U Q W 2811
OH
Chrysospermin_C * Ac F U S U J L Q G U U A A U P U U U Q W 2812
OH
Chrysospermin_D * Ac F U S U J L Q G U U A A U P J U U Q W 2813
OH
Clonostachin * Ac U O L J O L J O U J U O J I 2814
O[CH(CH(OH)CH2OH)CH(OH)CH(OH)CH2]OH
Emerimicin_II_A * Ac W I Q U I T U L U O Q U O U P F OH 2815
Emerimicin_II_B * Ac W I Q J I T U L U O Q U O U P F OH 2816
Emerimicin_III * Ac F U U U V G L U U O Q J O U F OH 2817
Emerimicin_IV * Ac F U U U V G L U U O Q J O A F OH 2818
Harzianin_HB_I * Ac U N L I U P J L U P L OH 2819
Harzianin_HC_I * Ac U N L U P S V U P U L U P L OH 2820
Harzianin_HC_III * Ac U N L U P S V U P J L U P L OH 2821
Harzianin_HC_IX * Ac U N L U P A I U P J L U P L OH 2822
Harzianin_HC_VI * Ac U N L U P A V U P U L U P L OH 2823
Harzianin_HC_VIII * Ac U N L U P A V U P J L U P L OH 2824
Harzianin_HC_VIII * Ac U N L U P A V U P J L U P L OH 2825
Harzianin_HC_X * Ac U Q L U P A V U P J L U P L OH 2826
Harzianin_HC_XI * Ac U N L U P S I U P U L U P L OH 2827
Harzianin_HC_XII * Ac U N L U P S I U P J L U P L OH 2828
Harzianin_HC_XIII * Ac U Q L U P S I U P J L U P L OH 2829
Harzianin_HC_XIV * Ac U N L U P A I U P U L U P L OH 2830
Harzianin_HC_XV * Ac U Q L U P A I U P J L U P L OH 2831
Harzianin_HK_VI * Ac U N I I U P L L U P L OH 2832
Harzianin_PCU4 * Ac U N L U P S I U P U L U P V OH 2833
Helioferin_A * Fa P ZZ A U I I U U AAE 2834
Helioferin_B * Fa P ZZ A U I I U U AMAE 2835
Heptaibin * Ac F U U U V G L U U O Q U O U F OH 2836
Hypelcin_A * Ac U P U A U U Q L U G U U U P V U U Q Q L 2837
OH
Hypelcin_A_I * Ac U P U A U U Q U L U G U U P V U U Q Q L 2838
OH
Hypelcin_A_II * Ac U P U A U A Q U L U G U U P V U U Q Q L 2839
OH
Hypelcin_A_III * Ac U P U A U U Q U L U G U U P V U U Q Q 2840
[C7H16NO]
Hypelcin_A_IV * Ac U P U A U U Q U I U G U U P V U U Q Q L 2841
OH
Hypelcin_A-III * Ac U P U A U U Q U L U G U U P V U J Q Q L 2842
OH
Hypelcin_A-IX * Ac U P U A U U Q U I U G U U P V U J Q Q L 2843
OH
Hypelcin_A-V * Ac U P U A U U Q U L U G U U P V U U Q Q I 2844
OH
Hypelcin_A-VI * Ac U P U A U A Q U L U G U U P V U U Q Q I 2845
OH
Hypelcin_A-VII * Ac U P U A U A Q U L U G U U P V U J Q Q L 2846
OH
Hypelcin_A-VIII * Ac U P U A U A Q U I U G U U P V U U Q Q L 2847
OH
Hypelcin_B_I * Ac U P U A U U Q U L U G U U P V U U E Q L 2848
OH
Hypelcin_B_II * Ac U P U A U A Q U L U G U U P V U U E Q L 2849
OH
Hypelcin_B_III * Ac U P U A U U Q U L U G U U P V U J E Q L 2850
OH
Hypelcin_B_IV * Ac U P U A U U Q U I U G U U P V U U E Q L 2851
OH
Hypelcin_B_V * Ac U P U A U U Q U L U G U U P V U U E Q I 2852
OH
Hypomurocin_A_I * Ac U Q V V U P L L U P L OH 2853
Hypomurocin_A_II * Ac J Q V V U P L L U P L OH 2854
Hypomurocin_A_III * Ac U Q V L U P L I U P L OH 2855
Hypomurocin_A_IV * Ac U Q I V U P L L U P L OH 2856
Hypomurocin_A_V * Ac U Q I I U P L L U P L OH 2857
Hypomurocin_A_Va * Ac U Q I L U P L I U P L OH 2858
Hypomurocin_B_I * Ac U S A L U Q U V U G U U P L U U Q V OH 2859
Hypomurocin_B_II * Ac U S A L U Q U V U G U U P L U U Q L OH 2860
Hypomurocin_B_IIIa * Ac U A A L U Q U V U G U U P L U U Q V OH 2861
Hypomurocin_B_IIIb * Ac U S A L U Q J V U G U U P L U U Q V OH 2862
Hypomurocin_B_IV * Ac U S A L U Q U V U G J U P L U U Q V OH 2863
Hypomurocin_B_V * Ac U S A L U Q U V U G J U P L U U Q L OH 2864
Leul_Zervamicin * Ac L I Q J I T U L U O Q U O U P F OH 2865
Longibrachin_A_I * Ac U A U A U A Q U V U G L U P V U U Q Q F 2866
OH
Longibrachin_A_II * Ac U A U A U A Q U V U G L U P V U J Q Q F 2867
OH
Longibrachin_A_III * Ac U A U A U U Q U V U G L U P V U U Q Q F 2868
OH
Longibrachin_A_IV * Ac U A U A U U Q U V U G L U P V U J Q Q F 2869
OH
Longibrachin_B_II * Ac U A U A U A Q U V U G L U P V U U E Q F 2870
OH
Longibrachin_B_III * Ac U A U A U A Q U V U G L U P V U J E Q F 2871
OH
LP237_F5 * Oc U P Y U Q Q U Zor Q A L OH 2872
LP237_F7 * Ac U P F U Q Q U U Q A L OH 2873
LP237_F8 * Oc U P F U Q Q U Zor Q A L OH 2874
NA_VII * Ac U A A U J Q U U U S L U OCH3 2875
Paracelsin_A * Ac U A U A U A Q U V U G U U P V U U Q Q 2876
F OH
Paracelsin_B * Ac U A U A U A Q U L U G U U P V U U Q Q F 2877
OH
Paracelsin_C * Ac U A U A U U Q U V U G U U P V U U Q Q 2878
F OH
Paracelsin_D * Ac U A U A U U Q U L U G U U P V U U Q Q F 2879
OH
Paracelsin_E * Ac U A U A U A Q U L U G U A P V U U Q Q F 2880
OH
Peptaibolin * Ac L U L U F OH 2881
Peptaivirin_A * Ac F U A U J L Q G U U A A U P J U U Q W 2882
OH
Peptaivirin_B * Ac F U S U J L Q G U U A A U P J U U Q F OH 2883
Polysporin_A * Ac U P U A U U Q U V U G V U P V U U Q Q F 2884
OH
Polysporin_B * Ac U P U A U U Q U V U G L U P V U U Q Q F 2885
OH
Polysporin_C * Ac U P U A U U Q U I U G L U P V U U Q Q F 2886
OH
Polysporin_D * Ac U P U A U U Q U I U G L U P V U V Q Q F 2887
OH
Pseudokinin_KLIII * Ac U N I I U P L L U P NH2 2888
Pseudokinin_KLVI * Ac U N I I U P L V hydroxyketopiperazine 2889
Samarosporin_I * Ac F U U U V G L U U O Q J O A F OH 2890
Samarosporin_II * Ac F U U U V G L U U O Q J O U F OH 2891
Saturnisporin_SA_I * Ac U A U A U A Q U L U G U U P V U U Q Q F 2892
OH
Saturnisporin_SA_II * Ac U A U A U A Q U L U G U U P V U J Q Q F 2893
OH
Saturnisporin_SA_III * Ac U A U A U U Q U L U G U U P V U U Q Q F 2894
OH
Saturnisporin_SA_IV * Ac U A U A U U Q U L U G U U P V U J Q Q F 2895
OH
Stilbellin_I * Ac F U U U V G L U U O Q J O A F OH 2896
Stilbellin_II * Ac F U U U V G L U U O Q J O U F OH 2897
Stilboflavin_A_1 * Ac U P U A U A Q U V U G U U P V U U E Q V 2898
OH
Stilboflavin_A_2 * Ac U P U A U A Q U L U G U U P V U U E Q V 2899
OH
Stilboflavin_A_3 * Ac U P U A U U Q U V U G U A P V U U E Q L 2900
OH
Stilboflavin_A_4 * Ac U P U A U A Q U L U G U U P V U U E Q L 2901
OH
Stilboflavin_A_5 * Ac U P U A U U Q U L U G U U P V U U E Q V 2902
OH
Stilboflavin_A_6 * Ac U P U A U A Q U L U G U U P V U U E Q J 2903
OH
Stilboflavin_A_7 * Ac U P U A U U Q U L U G U U P V U U E Q I 2904
OH
Stilboflavin_B_1 * Ac U P U A U A Q U V U G U U P V U U Q Q 2905
V OH
Stilboflavin_B_2 * Ac U P U A U A Q U L U G U U P V U U Q Q V 2906
OH
Stilboflavin_B_3 * Ac U P U A U A Q U V U G U U P V U U Q Q L 2907
OH
Stilboflavin_B_4 * Ac U P U A U A Q U L U G U U P V U U Q Q L 2908
OH
Stilboflavin_B_5 * Ac U P U A U U Q U L U G U U P V U U Q Q V 2909
OH
Stilboflavin_B_6 * Ac U P U A U U Q U V U G U U P V U U Q Q 2910
V OH
Stilboflavin_B_7 * Ac U P U A U U Q U L U G U U P V U U Q Q L 2911
OH
Stilboflavin_B_8 * Ac U P U A U U Q U V U G U U P V U U Q Q L 2912
OH
Stilboflavin_B_9 * Ac U P U A U U Q U L U G U U P V U U Q Q I 2913
OH
Stilboflavin_B_10 * Ac U P U A U U Q U V U G U U P V U U Q Q I 2914
OH
Suzukacillin * Ac U A U A U A Q U U U G L U P V U U Q Q F 2915
OH
Trichobrachin_A-I * Ac U N L L U P L U U P L OH 2916
Trichobrachin_A-II * Ac U N L L U P V L U P V OH 2917
Trichobrachin_A-III * Ac U N V L U P L L U P V OH 2918
Trichobrachin_A-IV * Ac U N L V U P L L U P V OH 2919
Trichobrachin_B-I * Ac U N L L U P V U V P L OH 2920
Trichobrachin_B-II * Ac U N V L U P L U V P L OH 2921
Trichobrachin_B-III * Ac U N L V U P L U V P L OH 2922
Trichobrachin_B-IV * Ac U N L L U P L U V P V OH 2923
Trichocellin_TC-A-I * Ac U A U A U A Q U L U G U U P V U U Q Q F 2924
OH
Trichocellin_TC-A-II * Ac U A U A U A Q U L U G U U P V U J Q Q F 2925
OH
Trichocellin_TC-A-III * Ac U A U A U A Q U I U G U U P V U U Q Q F 2926
OH
Trichocellin_TC-A-IV * Ac U A U A U A Q U I U G U U P V U J Q Q F 2927
OH
Trichocellin_TC-A-V * Ac U A U A U A Q U L U G L U P V U U Q Q F 2928
OH
Trichocellin_TC-A-VI * Ac U A U A U A Q U L U G L U P V U J Q Q F 2929
OH
Trichocellin_TC-A- * Ac U A U A U A Q U I U G L U P V U U Q Q F 2930
VII OH
Trichocellin_TC-A- * Ac U A U A U A Q U I U G L U P V U J Q Q F 2931
VIII OH
Trichocellin_TC-B-I * Ac U A U A U A Q U L U G U U P V U U E Q F 2932
OH
Trichocellin_TC-B-II * Ac U A U A U A Q U L U G U U P V U J E Q F 2933
OH
Trichodecenin_TD_I * (Z)-4-decenoyl G G L U G I L OH 2934
Trichodecenin_TD_II * (Z)-4-decenoyl G G L U G L L OH 2935
Trichogin_A_IV * Oc U G L U G G L U G I L OH 2936
Trichokindin_Ia * Ac U S A U U Q J L U A U U P L U U Q I OH 2937
Trichokindin_Ib * Ac U S A U J Q U L U A U U P L U U Q I OH 2938
Trichokindin_IIa * Ac U S A U U Q U L U A J U P L U U Q I OH 2939
Trichokindin_IIb * Ac U S A U J Q J L U A U U P L U U Q L OH 2940
Trichokindin_IIIa * Ac U S A U U Q J L U A J U P L U U Q L OH 2941
Trichokindin_IIIb * Ac U S A U J Q U L U A J U P L U U Q L OH 2942
Trichokindin_IV * Ac U S A U J Q J L U A U U P L U U Q I OH 2943
Trichokindin_Va * Ac U S A U U Q J L U A J U P L U U Q I OH 2944
Trichokindin_Vb * Ac U S A U J Q U L U A J U P L U U Q I OH 2945
Trichokindin_VI * Ac U S A U J Q J L U A J U P L U U Q L OH 2946
Trichokindin_VII * Ac U S A U J Q J L U A J U P L U U Q I OH 2947
Trichokonin_Ia * Ac U A U A U A Q U V U G L A P V U U Q Q F 2948
OH
Trichokonin_Ib * Ac U G U A U A Q U V U G L U P V U U Q Q F 2949
OH
Trichokonin_IIa * Ac U A U A U A Q U V U G L U P A U U Q Q F 2950
OH
Trichokonin_IIb * Ac A A U A U A Q U V U G L U P V U U Q Q F 2951
OH
Trichokonin_IIc * Ac U A A A U A Q U V U G L U P V U U Q Q F 2952
OH
Trichokonin_V * Ac U A U A U Q U V U G L U P V U U Q Q F 2953
OH
Trichokonin_VII * Ac U A U A U A Q U V U G L U P V U J Q Q F 2954
OH
Trichokonin_VIII * Ac U A U A U U Q U V U G L U P V U U Q Q F 2955
OH
Trichokonin_IX * Ac U A U A U A Q U V U G L U P V U J Q Q F 2956
OH
Tricholongin_BI * Ac U G F U U Q U U U S L U P V U U Q Q L 2957
OH
Tricholongin_BII * Ac U G F U U Q U U U S L U P V U J Q Q L 2958
OH
Trichopolyn_I * Fa P ZZ A U U I A U U AMAE 2959
Trichopolyn_II * Fa P ZZ A U U V A U U AMAE 2960
Trichopolyn_III * Fa P ZZ A U U I A U A AMAE 2961
Trichopolyn_IV * Fa P ZZ A U U V A U A AMAE 2962
Trichopolyn_V * Fa′ P ZZ A U U I A U U AMAE 2963
Trichorovin_TV_Ia * Ac U N V Lx U P Lx Lx U P V OH 2964
Trichorovin_TV_Ib * Ac U N V V U P Lx Lx U P Lx OH 2965
Trichorovin_TV_IIa * Ac U N V V U P Lx Lx U P Lx OH 2966
Trichorovin_TV_IIb * Ac U N Lx V U P Lx Lx U P V OH 2967
Trichorovin_TV_IIIa * Ac U Q V V U P Lx Lx U P Lx OH 2968
Trichorovin_TV_IIIb * Ac U Q V Lx U P Lx Lx U P V OH 2969
Trichorovin_TV_IVa * Ac U Q V V U P Lx Lx U P Lx OH 2970
Trichorovin_TV_IVb * Ac U Q Lx V U P Lx Lx U P V OH 2971
Trichorovin_TV_IVc * Ac U N V Lx U P Lx Lx U P Lx OH 2972
Trichorovin_TV_IXa * Ac U Q V Lx U P Lx Lx U P Lx OH 2973
Trichorovin_TV_IXb * Ac U Q Lx Lx U P Lx Lx U P V OH 2974
Trichorovin_TV_Va * Ac U N V Lx U P Lx Lx U P Lx OH 2975
Trichorovin_TV_Vb * Ac U N Lx Lx U P Lx Lx U P V OH 2976
Trichorovin_TV_VIa * Ac U N V Lx U P Lx Lx U P Lx OH 2977
Trichorovin_TV_VIb * Ac U N Lx Lx U P Lx Lx U P V OH 2978
Trichorovin_TV_VIIa * Ac U N Lx V U P Lx Lx U P Lx OH 2979
Trichorovin_TV_VIIb * Ac U Q V Lx U P Lx Lx U P V OH 2980
Trichorovin_TV_VIII * Ac U Q V Lx U P Lx Lx U P Lx OH 2981
Trichorovin_TV_Xa * Ac U Q Lx V U P Lx Lx U P Lx OH 2982
Trichorovin_TV_Xb * Ac U N Lx Lx U P Lx Lx U P Lx OH 2983
Trichorovin_TV_XIIa * Ac U N I I U P L L U P I OH 2984
Trichorovin_TV_XIIb * Ac U N Lx Lx U P Lx Lx U P L OH 2985
Trichorovin_TV_XIII * Ac U Q Lx Lx U P Lx Lx U P Lx OH 2986
Trichorovin_TV_XIV * Ac U Q Lx Lx U P Lx Lx U P Lx OH 2987
Trichorozin_I * Ac U N I L U P I L U P V OH 2988
Trichorozin_II * Ac U Q I L U P I L U P V OH 2989
Trichorozin_III * Ac U N I L U P I L U P L OH 2990
Trichorozin_IV * Ac U Q I L U P I L U P L OH 2991
Trichorzianine_TA_IIIc * Ac U A A U U Q U U U S L U P V U I Q Q W 2992
OH
Trichorzianine_TB_IIa * Ac U A A U U Q U U U S L U P L U I Q E W 2993
OH
Trichorzianine_TB_IIIc * Ac U A A U U Q U U U S L U P V U I Q E W 2994
OH
Trichorzianine_TB_IVb * Ac U A A U J Q U U U S L U P V U I Q E W 2995
OH
Trichorzianine_TB_Vb * Ac U A A U U Q U U U S L U P L U I Q E F OH 2996
Trichorzianine_TB_VIa * Ac U A A U J Q U U U S L U P L U I Q E F OH 2997
Trichorzianine_TB_VIb * Ac U A A U U Q U U U S L U P V U I Q E F 2998
OH
Trichorzianine_TB_VII * Ac U A A U J Q U U U S L U P V U I Q E F OH 2999
Trichorzin_HA_I * Ac U G A U U Q U V U G L U P L U U Q L OH 3000
Trichorzin_HA_II * Ac U G A U U Q U V U G L U P L U J Q L OH 3001
Trichorzin_HA_III * Ac U G A U J Q U V U G L U P L U U Q L OH 3002
Trichorzin_HA_V * Ac U G A U J Q U V U G L U P L U J Q L OH 3003
Trichorzin_HA_VI * Ac U G A U J Q J V U G L U P L U J Q L OH 3004
Trichorzin_HA_VII * Ac U G A U J Q V V U G L U P L U J Q L OH 3005
Trichorzin_MA_I * Ac U S A U U Q U L U G L U P L U U Q V OH 3006
Trichorzin_MA_II * Ac U S A U J Q U L U G L U P L U U Q V OH 3007
Trichorzin_MA_III * Ac U S A U J Q J L U G L U P L U U Q V OH 3008
Trichorzin_PA_II * Ac U S A U J Q U V U G L U P L U U Q W OH 3009
Trichorzin_PA_IV * Ac U S A U J Q J V U G L U P L U U Q W OH 3010
Trichorzin_PA_V * Ac U S A J J Q U V U G L U P L U U Q W OH 3011
Trichorzin_PA_VI * Ac U S A U J Q U V U G L U P L U U Q F OH 3012
Trichorzin_PA_VII * Ac U S A J J Q U V U G L U P L U U Q W OH 3013
Trichorzin_PA_VIII * Ac U S A U J Q J V U G L U P L U U Q F OH 3014
Trichorzin_PA_IX * Ac U S A J J Q U V U G L U P L U U Q F OH 3015
Trichorzin_PAU4 * Ac U S A U U Q U V U G L U P L U U Q W OH 3016
Trichosporin_TS-B- * Ac U A G U A U Q U Lx A A Vx A P V U Vx Q 3017
1a-1 Q F OH
Trichosporin_TS-B- * Ac U A G A U U Q U Lx A A Vx A P V U Vx Q 3018
1a-2 Q F OH
Trichosporin_TS-B- * Ac U A G A U U Q U Lx U G Lx A P V U A Q 3019
1b Q F OH
Trichosporin_TS-B- * Ac U A S A U U Q U Lx U G Lx A P V U U Q Q 3020
1d F OH
Trichosporin_TS-B- * Ac U A G A U U Q U Lx U G Lx U P V U U Q 3021
1e Q F OH
Trichosporin_TS-B-1f * Ac U A S A U U Q U Lx U G Lx U P V U U Q Q 3022
F OH
Trichosporin_TS-B- * Ac U A G A U U Q U Lx U G Lx A P V U U Q 3023
1g Q F OH
Trichosporin_TS-B- * Ac U A G A U U Q U Lx U G Lx U P V U Vx Q 3024
1h Q F OH
Trichosporin_TS-B-Ia * Ac U A S A U U Q U L U G L U P V U U Q Q F 3025
OH
Trichosporin_TS-B- * Ac U A A A U U Q U L U G L U P V U U Q Q F 3026
IIIa OH
Trichosporin_TS-B- * Ac U A A A U U Q U I U G L U P V U A Q Q F 3027
IIIb OH
Trichosporin_TS-B- * Ac U A A A A U Q U I U G L U P V U U Q Q F 3028
IIIc OH
Trichosporin_TS-B- * Ac U A A A U U Q U V U G L U P V U U Q Q F 3029
IIId OH
Trichosporin_TS-B- * Ac U A A A U U Q U L U G L U P V U J Q Q F 3030
IVb OH
Trichosporin_TS-B- * Ac U A U A U U Q U V U G L U P V U U Q Q F 3031
IVc OH
Trichosporin_TS-B- * Ac U A A A U U Q U V U G L U P V U J Q Q F 3032
IVd OH
Trichosporin_TS-B-V * Ac U A A A U U Q U I U G L U P V U U Q Q F 3033
OH
Trichosporin_TS-B- * Ac U A U A U U Q U I U G L U P V U U Q Q F 3034
VIa OH
Trichosporin_TS-B- * Ac U A A A U U Q U I U G L U P V U J Q Q F 3035
VIb OH
Trichotoxin_A-40 * Ac U G U L U E U U U A U U P L U J Q V OH 3036
Trichotoxin_A-40_I * Ac U G U L U Q U U A A U U P L U U E V OH 3037
Trichotoxin_A-40_II * Ac U G U L U Q U U U A A U P L U U E V OH 3038
Trichotoxin_A-40_III * Ac U G U L U Q U U A A U U P L U J E V OH 3039
Trichotoxin_A-40_IV * Ac U G U L U Q U U U A U U P L U U E V OH 3040
Trichotoxin_A-40_V * Ac U G U L U Q U U U A U U P L U J E V OH 3041
Trichotoxin_A-40_Va * Ac U A U L U Q U U U A U U P L U U E V OH 3042
Trichotoxin_A-50_E * Ac U G U L U Q U U U A A U P L U U Q V OH 3043
Trichotoxin_A-50_F * Ac U G U L U Q U U A A A U P L U J Q V OH 3044
Trichotoxin_A-50_G * Ac U G U L U Q U U U A A U P L U J Q V OH 3045
Trichotoxin_A-50_H * Ac U A U L U Q U U U A A U P L U J Q V OH 3046
Trichotoxin_A-50_I * Ac U G U L U Q U U U A U U P L U J Q V OH 3047
Trichotoxin_A-50_J * Ac U A U L U Q U U U A U U P L U J Q V OH 3048
Trichovirin-Ia * Ac U G A L A Q Vx V U G U U P L U U Q L 3049
OH
Trichovirin-Ib * Ac U G A L U Q A V U G J U P L U U Q L OH 3050
Trichovirin-IIa * Ac U G A L A Q U V U G J U P L U U Q L OH 3051
Trichovirin-IIb * Ac U G A L U Q U V U G U U P L U U Q L OH 3052
Trichovirin-IIc * Ac U G A L U Q Vx V U G U U P L U U Q L 3053
OH
Trichovirin-IIIa * Ac U G A L U Q J V U G U U P L U U Q L OH 3054
Trichovirin-IIIb * Ac U G A L J Q J U U G U U P L U U Q L OH 3055
Trichovirin-IVa * Ac U G A L J Q J V U G U U P L U U Q L OH 3056
Trichovirin-IVb * Ac U G A L U Q U V U G J U P L U U Q L OH 3057
Trichovirin-V * Ac U G A L U Q J V U G J U P L U U Q L OH 3058
Trichovirin-VIa * Ac U G A L U Q J L U G J U P L U U Q L OH 3059
Trichovirin-VIb * Ac U G A L J Q J V U G J U P L U U Q L OH 3060
Trikoningin_KA_V * Ac U G A U I Q U U U S L U P V U I Q Q L OH 3061
Trikoningin_KB_I * Oc U G V U G G V U G I L OH 3062
Trikoningin_KB_II * Oc J G V U G G V U G I L OH 3063
Tylopeptin_A * Ac W V U J A Q A U S U A L U Q L OH 3064
Tylopeptin_B * Ac W V U U A Q A U S U A L U Q L OH 3065
XR586 * Ac W J Q U I T U L U P Q U O J P F G OH 3066
Zervamicin_A-1-16 * Boc W I A U I V U L U P A U P U P F OCH3 3067
Zervamicin_ZIA * Ac W I E J V T U L U O Q U O U P F OH 3068
Zervamicin_ZIB * Ac W V E J I T U L U O Q U O U P F OH 3069
Zervamicin_ZIB′ * Ac W I E U I T U L U O Q U O U P F OH 3070
Zervamicin_ZIC * Ac W I E J I T U L U O Q U O U P F OH 3071
Zervamicin_ZII-1 * Ac W I Q U V T U L U O Q U O U P F OH 3072
Zervamicin_ZII-2 * Ac W I Q U I T U V U O Q U O U P F OH 3073
Zervamicin_ZII-3 * Ac W V Q U I T U L U O Q U O U P F OH 3074
Zervamicin_ZII-4 * Ac W I Q J V T U L U O Q U O U P F OH 3075
Zervamicin_ZII-5 * Ac W I Q J I T U V U O Q U O U P F OH 3076
Zervamicin_ZIIA * Ac W I Q U I T U L U O Q U O U P F OH 3077
Zervamicin_ZIIB * Ac W I Q J I T U L U O Q U O U P F OH 3078
CAMEL135 GWRLIKKILRVFKGL 3079
(CAM135)
Novispirin G2 KNLRIIRKGIHIIKKY* 3080
B-33 FKKFWKWFRRF 3081
B-34 LKRFLKWFKRF 3082
B-35 KLFKRWKHLFR 3083
B-36 RLLKRFKHLFK 3084
B-37 FKTFLKWLHRF 3085
B-38 IKQLLHFFQRF 3086
B-39 KLLQTFKQIFR 3087
B-40 RILKELKNLFK 3088
B-41 LKQFVHFIHRF 3089
B-42 VKTLLHIFQRF 3090
B-43 KLVEQLKEIFR 3091
B-44 RVLQEIKQILK 3092
B-45 VKNLAELVHRF 3093
B-46 ATHLLHALQRF 3094
B-47 KLAENVKEILR 3095
B-48 RALHEAKEALK 3096
B-49 FHYFWHWFHRF 3097
B-50 LYHFLHWFQRF 3098
B-51 YLFQTWQHLFR 3099
B-52 YLLTEFQHLFK 3100
B-53 FKTFLQWLHRF 3101
B-54 IKTLLHFFQRF 3102
B-55 KLLQTFNQIFR 3103
B-56 TILQSLKNIFK 3104
B-57 LKQFVKFIHRF 3105
B-58 VKQLLKIFNRF 3106
B-59 KLVQQLKNIFR 3107
B-60 RVLNQVKQILK 3108
B-61 VKKLAKLVRRF 3109
B-62 AKRLLKVLKRF 3110
B-63 KLAQKVKRVLR 3111
B-64 RALKRIKHVLK 3112
1C-1 RRRRWWW 3113
1C-2 RRWWRRW 3114
1C-3 RRRWWWR 3115
1C-4 RWRWRWR 3116
2C-1 RRRFWWR 3117
2C-2 RRWWRRF* 3118
2C-3 RRRWWWF* 3119
2C-4 RWRWRWF* 3120
3C-1 RRRRWWK 3121
3C-2 RRWWRRK 3122
3C-3 RRRWWWK 3123
3C-4 RWRWRWK 3124
4C-1 RRRKWWK 3125
4C-2 RRWKRRK 3126
4C-3 RRRKWWK 3127
4C-4 RWRKRWK 3128
a-3 LHLLHQLLHLLHQF* 3129
a-4 AQAAHQAAHAAHQF* 3130
a-5 KLKKLLKKLKKLLK 3131
a-6 LKLLKKLLKLLKKF* 3132
a-7 LQLLKQLLKLLKQF* 3133
a-8 AQAAKQAAKAAKQF* 3134
a-9 RWRRWWRHFHHFFH* 3135
a-10 KLKKLLKRWRRWWR 3136
a-11 RWRRLLKKLHHLLH* 3137
a-12 KLKKLLKHLHHLLH* 3138
BD-1 FVF RHK WVW KHR FLF 3139
BD-2 VFI HRH VWV HKH VLF 3140
BD-3 WR WR AR WR WR LR WR F 3141
BD-4 WR IH LR AR LH VK FR F 3142
BD-5 LR IH AR FK VH IR LK F 3143
BD-6 FH IK FR VH LK VR FH F 3144
BD-7 FH VK IH FR LH VK FH F 3145
BD-8 LH IH AH FH VH IH LH F 3146
BD-9 FK IH FR LK VH IR FK F 3147
BD-10 FK AH IR FK LR VK FH F 3148
BD-11 LK AK IK FK VK LK IK F 3149
BD-12 WIW KHK FL HRH FLF 3150
BD-13 VFL HRH VI KHK LVF 3151
BD-14 FL HKH VL RHR IVF 3152
BD-15 VF KHK IV HRH ILF 3153
BD-16 FLF KH LFL HR IFF 3154
BD-17 LF KH ILI HR VIF 3155
BD-18 FL HKH LF KHK LF 3156
BD-19 VF RHR FI HRH VF 3157
BD-20 FI HK LV HKH VLF 3158
BD-21 VL RH LF RHR IVF 3159
BD-22 LV HK LIL RH LLF 3160
BD-23 VF KR VLI HK LIF 3161
BD-24 IV RK FLF RHK VF 3162
BD-25 VL KH VIA HKR LF 3163
BD-26 FI RK FLF KH LF 3164
BD-27 VI RH VWV RK LF 3165
BD-28 FLF RHR F RHR LVF 3166
BD-29 LFL HKH A KHK FLF 3167
BD-30 F KHK F KHK FIF 3168
BD-31 L RHR L RHR LIF 3169
BD-32 LIL K FLF K FVF 3170
BD-33 VLI R ILV R VIF 3171
BD-34 F RHR F RHR F 3172
BD-35 L KHK L KHK F 3173
BD-36 F K F KHK LIF 3174
BD-37 L R L RHR VLF 3175
BD-38 F K FLF K FLF 3176
BD-39 L R LFL R WLF 3177
BD-40 F K FLF KHK F 3178
BD-41 L R LFL RHR F 3179
BD-42 F K FLF K F 3180
BD-43 L R LFL R F 3181
AA-1 HHFFHHFHHFFHHF* 3182
AA-2 FHFFHHFFHFFHHF* 3183
AA-3 KLLK-GAT-FHFFHHFFHFFHHF 3184
AA-4 KLLK-FHFFHHFFHFFHHF 3185
AA-5 FHFFHHFFHFFHHFKLLK 3186
RIP YSPWTNF* 3187
Lariatin A c(Gly-Ser-Gln-Leu-Val-Tyr-Arg-Glu)-Trp-Val- 3188
(anti-mycobacteria) Gly-His-Ser-Asn-Val-Ile-Lys-Pro
Lariatin B c(Gly-Ser-Gln-Leu-Val-Tyr-Arg-Glu)-Trp-Val- 3189
(anti-mycobacteria) Gly-His-Ser-Asn-Val-Ile-Lys-Gly-Pro-Pro
Abreviations:
U - Aminoisobutyric Acid (Aib);
J - Isovaline (Iva);
O - Hydroxyproline (Hyp);
Z - Ethylnorvaline (EtNor);
x or xx means L or I at that position;
Ac - optionally acetylated N-term;
OH, OCH3 - optional C-term;
Alkane long chains are noted in brackets;
*optionally amidated C-terminus. Where protecting groups are shown, the gropus are optional. Conversely any of the peptides shown without protecting groups can, optionally bear one or more protecting groups. Where peptides are shown circularized, linear forms are also contemplated. Conversely, where linear peptides are shown circularlized versions are also contemplated.
In certain embodiments the antimicrobial peptide consists of or comprises the amino acid sequence of LL-37 (LLGDFFRK SKEKIGKEFKRIVQRIKD FLRNL VPRTES, SEQ ID NO:3190) or a variant of LL-37. LL-37 is a cathelicidin anti-microbial corresponding to amino acids 134-170 of the human cationic antimicrobial protein 18 (hCAP18). In certain embodiments the antimicrobial peptide consists of or comprises the amino acid sequence of an LL-37 variant as described in U.S. Patent Publication No: 2009/0156499 A1). Illustrative variants comprise or consist of the amino acid sequence having at least 90%, 95%, or 98% sequence identity with the amino acid sequence FKRIVQRIKDFLRX1 (SEQ ID NO:3191), where Xi is selected from the group consisting of 0, 1, 2, 3, 4, 5, 6, 7, and 8 amino acids. In certain embodiments illustrative variants comprise or consist of the amino acid sequence having at least 90%, 95%, or 98% sequence identity with the amino acid sequence XiRLFDKIRQVIRKFX2 (SEQ ID NO:3192) where Xi is 0, 1, 2, 3, 4, 5, 6, 7, or 8 amino acids and X2 is 0, 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11, 12, 13, 14, 15, or 16 amino acids.
In certain embodiments the antimicrobial peptide consists of or comprises the amino acid sequence of an LL-37 variant shown in Table 15.
TABLE 15
LL-37 peptide and variants.
SEQ
ID Amino acid sequence ID NO
LL-37 LLGDFFRKSKEKIGKEFKRIVQRIKDFLRN 3193
LVPRTES
Cys-LL-37 CLLGDFFRKSKEKIGKEFKRIVQRIKDFLR 3194
NLVPRTES
LL-37(17-32) FKRIVQRIKDFLRNLV 3195
Cys-LL-37-Cys CLLGDFFRKSKEKIGKEFKRIVQRIKDFLR 3196
NLVPRTESC
LL-37FK-13 FKRIVQRIKDFLR 3197
LL-37FKR FKRIVQRIKDFLRNLVPRTES 3198
LL-37GKE GKEFKRIVQRIKDFLRNLVPR 3199
LL-37KRI KRIVQRIKDFLRNLVPRTES 3200
LL-37LLG LLGDFFRKSKEKIGKEFKRIV 3201
LL-37RKS RKSKEKIGKEFKRIVQRIKDFLRNLVPRTES 3202
LL-37SKE SKEKIGKEFKRIVQRIKDFLR 3203
LL-37-Cys LLGDFFRKSKEKIGKEFKRIVQRIKDFLRN 3204
LVPRTESC
A number of antimicrobial peptides are also disclosed in U.S. Pat. Nos. 7,271,239, 7,223,840, 7,176,276, 6,809,181, 6,699,689, 6,420,116, 6,358,921, 6,316,594, 6,235,973, 6,183,992, 6,143,498, 6,042,848, 6,040,291, 5,936,063, 5,830,993, 5,428,016, 5,424,396, 5,032,574, 4,623,733, which are incorporated herein by reference for the disclosure of particular antimicrobial peptides.
v. Ligands.
In certain embodiments the effector can comprise one ore more ligands, epitope tags, and/or antibodies. In certain embodiments preferred ligands and antibodies include those that bind to surface markers on immune cells. Chimeric moieties utilizing such antibodies as effector molecules act as bifunctional linkers establishing an association between the immune cells bearing binding partner for the ligand or antibody and the target microorganism(s).
The terms “epitope tag” or “affinity tag” are used interchangeably herein, and used refers to a molecule or domain of a molecule that is specifically recognized by an antibody or other binding partner. The term also refers to the binding partner complex as well. Thus, for example, biotin or a biotin/avidin complex are both regarded as an affinity tag. In addition to epitopes recognized in epitope/antibody interactions, affinity tags also comprise “epitopes” recognized by other binding molecules (e.g. ligands bound by receptors), ligands bound by other ligands to form heterodimers or homodimers, His6 bound by Ni-NTA, biotin bound by avidin, streptavidin, or anti-biotin antibodies, and the like.
Epitope tags are well known to those of skill in the art. Moreover, antibodies specific to a wide variety of epitope tags are commercially available. These include but are not limited to antibodies against the DYKDDDDK (SEQ ID NO:3205) epitope, c-myc antibodies (available from Sigma, St. Louis), the HNK-1 carbohydrate epitope, the HA epitope, the HSV epitope, the His4 (SEQ ID NO:3206), His5 (SEQ ID NO:3207), and His6 (SEQ ID NO:3208) epitopes that are recognized by the His epitope specific antibodies (see, e.g., Qiagen), and the like. In addition, vectors for epitope tagging proteins are commercially available. Thus, for example, the pCMV-Tag1 vector is an epitope tagging vector designed for gene expression in mammalian cells. A target gene inserted into the pCMV-Tag1 vector can be tagged with the FLAG ® epitope (N-terminal, C-terminal or internal tagging), the c-myc epitope (C-terminal) or both the FLAG (N-terminal) and c-myc (C-terminal) epitopes.
vi. Lipids and Liposomes.
In certain embodiments the effectors comprise one or more microparticles or nanoparticles that can be loaded with an effector agent (e.g., a pharmaceutical, a label, etc.). In certain embodiments the microparticles or nanoparticles are lipidic particles. Lipidic particles are microparticles or nanoparticles that include at least one lipid component forming a condensed lipid phase. Typically, a lipidic nanoparticle has preponderance of lipids in its composition. Various condensed lipid phases include solid amorphous or true crystalline phases; isomorphic liquid phases (droplets); and various hydrated mesomorphic oriented lipid phases such as liquid crystalline and pseudocrystalline bilayer phases (L-alpha, L-beta, P-beta, Lc), interdigitated bilayer phases, and nonlamellar phases (see, e.g., The Structure of Biological Membranes, ed. by P. Yeagle, CRC Press, Bora Raton, Fla., 1991). Lipidic microparticles include, but are not limited to a liposome, a lipid-nucleic acid complex, a lipid-drug complex, a lipid-label complex, a solid lipid particle, a microemulsion droplet, and the like. Methods of making and using these types of lipidic microparticles and nanoparticles, as well as attachment of affinity moieties, e.g., antibodies, to them are known in the art (see, e.g., U.S. Pat. Nos. 5,077,057; 5,100,591; 5,616,334; 6,406,713; 5,576,016; 6,248,363; Bondi et al. (2003) Drug Delivery 10: 245-250; Pedersen et al., (2006) Eur. J. Pharm. Biopharm. 62: 155-162, 2006 (solid lipid particles); U.S. Pat. Nos. 5,534,502; 6,720,001; Shiokawa et al. (2005) Clin. Cancer Res. 11: 2018-2025 (microemulsions); U.S. Pat. Nos. 6,071,533 (lipid-nucleic acid complexes), and the like).
A liposome is generally defined as a particle comprising one or more lipid bilayers enclosing an interior, typically an aqueous interior. Thus, a liposome is often a vesicle formed by a bilayer lipid membrane. There are many methods for the preparation of liposomes. Some of them are used to prepare small vesicles (d<0.05 micrometer), some for larger vesicles (d>0.05 micrometer). Some are used to prepare multilamellar vesicles, some for unilamellar ones. Methods for liposome preparation are exhaustively described in several review articles such as Szoka and Papahadjopoulos (1980) Ann. Rev. Biophys. Bioeng., 9: 467, Deamer and Uster (1983) Pp. 27-51 In: Liposomes, ed. M. J. Ostro, Marcel Dekker, New York, and the like.
In various embodiments the liposomes include a surface coating of a hydrophilic polymer chain. “Surface-coating” refers to the coating of any hydrophilic polymer on the surface of liposomes. The hydrophilic polymer is included in the liposome by including in the liposome composition one or more vesicle-forming lipids derivatized with a hydrophilic polymer chain. In certain embodiments, vesicle-forming lipids with diacyl chains, such as phospholipids, are preferred. One illustrative phospholipid is phosphatidylethanolamine (PE), which contains a reactive amino group convenient for coupling to the activated polymers. One illustrative PE is distearoyl PE (DSPE). Another example is non-phospholipid double chain amphiphilic lipids, such as diacyl- or dialkylglycerols, derivatized with a hydrophilic polymer chain.
In certain embodiments a hydrophilic polymer for use in coupling to a vesicle forming lipid is polyethyleneglycol (PEG), preferably as a PEG chain having a molecular weight between 1,000-10,000 Daltons, more preferably between 1,000-5,000 Daltons, most preferably between 2,000-5,000 Daltons. Methoxy or ethoxy-capped analogues of PEG are also useful hydrophilic polymers, commercially available in a variety of polymer sizes, e.g., 120-20,000 Daltons.
Other hydrophilic polymers that can be suitable include, but are not limited to polylactic acid, polyglycolic acid, polyvinylpyrrolidone, polymethyloxazoline, polyethyloxazoline, polyhydroxypropyl methacrylamide, polymethacrylamide, polydimethylacrylamide, and derivatized celluloses, such as hydroxymethylcellulose or hydroxyethylcellulose.
Preparation of lipid-polymer conjugates containing these polymers attached to a suitable lipid, such as PE, have been described, for example in U.S. Pat. No. 5,395,
The liposomes can, optionally be prepared for attachment to one or more targeting moieties described herein. Here the lipid component included in the liposomes would include either a lipid derivatized with the targeting moiety, or a lipid having a polar-head chemical group, e.g., on a linker, that can be derivatized with the targeting moiety in preformed liposomes, according to known methods.
Methods of functionalizing lipids and liposomes with affinity moieties such as antibodies are well known to those of skill in the art (see, e.g. , DE 3,218,121; Epstein et al. (1985) Proc. Natl. Acad. Sci., USA, 82:3688 (1985); Hwang et al. (1980) Proc. Natl. Acad. Sci., USA, 77: 4030; EP 52,322; EP 36,676; EP 88,046; EP 143,949; EP 142,641; Japanese patent application 83-118008; U.S. Pat. Nos. 4,485,045 and 4,544,545; and EP 102,324, all of which are incorporated herein by reference).
vii. Agents That Physically Disrupt the Extracellular Matrix Within a Community of Microorganisms
In certain embodiments, peptides can be coupled to agents that physically disrupt the extracellular matrix within a community of microorganisms, for example a biofilm. In certain preferred embodiments, such an agent could be a bacterial cell-wall degrading enzyme, for example SAL-2, or any species of glycosidase, alginase, peptidase, proteinase, lipase, or DNA or RNA degrading enzyme or compound, for example rhRNase. Disruption of extracellular matrix of biofilms can result in clearance and therapeutic benefit.
Peptides can also be attached to antimicrobial proteins, such as Protein Inhibitor C or Colicin, or fragments thereof, for example the IIa domain of Colicin, or the heparin-binding domain of Protein Inhibitor C.
viii. Polymeric microparticles and/or Nanoparticles.
In certain embodiments the effector(s) comprise polymeric microparticles and/or nanoparticles and/or micelles.
Microparticle and nanoparticle-based drug delivery systems have considerable potential for treatment of various microorganisms. Technological advantages of polymeric microparticles or nanoparticles used as drug carriers are high stability, high carrier capacity, feasibility of incorporation of both hydrophilic and hydrophobic substances, and feasibility of variable routes of administration, including oral application and inhalation. Polymeric nanoparticles can also be designed to allow controlled (sustained) drug release from the matrix. These properties of nanoparticles enable improvement of drug bioavailability and reduction of the dosing frequency.
Polymeric nanoparticles are typically micron or submicron (<1 μm) colloidal particles. This definition includes monolithic nanoparticles (nanospheres) in which the drug is adsorbed, dissolved, or dispersed throughout the matrix and nanocapsules in which the drug is confined to an aqueous or oily core surrounded by a shell-like wall. Alternatively, in certain embodiments, the drug can be covalently attached to the surface or into the matrix.
Polymeric microparticles and nanoparticles are typically made from biocompatible and biodegradable materials such as polymers, either natural (e.g., gelatin, albumin) or synthetic (e.g., polylactides, polyalkylcyanoacrylates), or solid lipids. In the body, the drug loaded in nanoparticles is usually released from the matrix by diffusion, swelling, erosion, or degradation. One commonly used material is poly(lactide-co-glycolide) (PLG).
Methods of fabricating and loading polymeric nanoparticles or microparticles are well known to those of skill in the art. Thus, for example, Matsumoto et al. (1999) Intl. J. Pharmaceutics, 185: 93-101 teaches the fabrication of poly(L-lactide)-poly(ethylene glycol)-poly(L-lactide) nanoparticles, Chawla et al. (2002) Intl. J. Pharmaceutics 249: 127-138, teaches the fabrication and use of poly(e-caprolactone) nanoparticles delivery of tamifoxen, and Bodmeier et al. (1988) Intl. J. Pharmaceutics, 43: 179-186, teaches the preparation of poly(D,L-lactide) microspheres using a solvent evaporation method. “Intl. J. Pharmaceutics, 1988, 43, 179-186. Other nanoparticle formulations are described, for example, by Williams et al. (2003) J. Controlled Release, 91: 167-172; Leroux et al. (1996) J. Controlled Release, 39: 339-350; Soppimath et al. (2001) J. Controlled Release, 70: 1-20; Brannon-Peppas (1995) Intl. J. Pharmaceutics, 116: 1-9; and the like.
C) Peptide Preparation.
The peptides described herein can be chemically synthesized using standard chemical peptide synthesis techniques or, particularly where the peptide does not comprise “D” amino acid residues, the peptide can be recombinantly expressed. Where the “D” polypeptides are recombinantly expressed, a host organism (e.g. bacteria, plant, fungal cells, etc.) can be cultured in an environment where one or more of the amino acids is provided to the organism exclusively in a D form. Recombinantly expressed peptides in such a system then incorporate those D amino acids.
In certain embodiments, D amino acids can be incorporated in recombinantly expressed peptides using modified amino acyl-tRNA synthetases that recognize D-amino acids.
In certain embodiments the peptides are chemically synthesized by any of a number of fluid or solid phase peptide synthesis techniques known to those of skill in the art. Solid phase synthesis in which the C-terminal amino acid of the sequence is attached to an insoluble support followed by sequential addition of the remaining amino acids in the sequence is a preferred method for the chemical synthesis of the polypeptides of this invention. Techniques for solid phase synthesis are well known to those of skill in the art and are described, for example, by Barany and Merrifield (1963) Solid-Phase Peptide Synthesis; pp. 3-284 in The Peptides: Analysis, Synthesis, Biology. Vol. 2: Special Methods in Peptide Synthesis, Part A.; Merrifield et al. (1963) J. Am. Chem. Soc., 85: 2149-2156, and Stewart et al. (1984) Solid Phase Peptide Synthesis, 2nd ed. Pierce Chem. Co., Rockford, Ill.
In one embodiment, the peptides can be synthesized by the solid phase peptide synthesis procedure using a benzhyderylamine resin (Beckman Bioproducts, 0.59 mmol of NH2/g of resin) as the solid support. The COOH terminal amino acid (e.g., t-butylcarbonyl-Phe) is attached to the solid support through a 4-(oxymethyl)phenacetyl group. This is a more stable linkage than the conventional benzyl ester linkage, yet the finished peptide can still be cleaved by hydrogenation. Transfer hydrogenation using formic acid as the hydrogen donor can be used for this purpose.
It is noted that in the chemical synthesis of peptides, particularly peptides comprising D amino acids, the synthesis usually produces a number of truncated peptides in addition to the desired full-length product. Thus, the peptides are typically purified using, e.g., HPLC.
D-amino acids, beta amino acids, non-natural amino acids, and the like can be incorporated at one or more positions in the peptide simply by using the appropriately derivatized amino acid residue in the chemical synthesis. Modified residues for solid phase peptide synthesis are commercially available from a number of suppliers (see, e.g., Advanced Chem Tech, Louisville; Nova Biochem, San Diego; Sigma, St Louis; Bachem California Inc., Torrance, etc.). The D-form and/or otherwise modified amino acids can be completely omitted or incorporated at any position in the peptide as desired. Thus, for example, in certain embodiments, the peptide can comprise a single modified acid, while in other embodiments, the peptide comprises at least two, generally at least three, more generally at least four, most generally at least five, preferably at least six, more preferably at least seven or even all modified amino acids. In certain embodiments, essentially every amino acid is a D-form amino acid.
As indicated above, the peptides and/or fusion proteins of this invention can also be recombinantly expressed. Accordingly, in certain embodiments, the antimicrobial peptides and/or targeting moieties, and/or fusion proteins of this invention are synthesized using recombinant expression systems. Generally this involves creating a DNA sequence that encodes the desired peptide or fusion protein, placing the DNA in an expression cassette under the control of a particular promoter, expressing the peptide or fusion protein in a host, isolating the expressed peptide or fusion protein and, if required, renaturing the peptide or fusion protein.
DNA encoding the peptide(s) or fusion protein(s) described herein can be prepared by any suitable method as described above, including, for example, cloning and restriction of appropriate sequences or direct chemical synthesis.
This nucleic acid can be easily ligated into an appropriate vector containing appropriate expression control sequences (e.g. promoter, enhancer, etc.), and, optionally, containing one or more selectable markers (e.g. antibiotic resistance genes).
The nucleic acid sequences encoding the peptides or fusion proteins described herein can be expressed in a variety of host cells, including, but not limited to, E. coli, other bacterial hosts, yeast, fungus, and various higher eukaryotic cells such as insect cells (e.g. SF3), the COS, CHO and HeLa cells lines and myeloma cell lines. The recombinant protein gene will typically be operably linked to appropriate expression control sequences for each host. For E. coli this can include a promoter such as the T7, trp, or lambda promoters, a ribosome binding site and preferably a transcription termination signal. For eukaryotic cells, the control sequences can include a promoter and often an enhancer (e.g., an enhancer derived from immunoglobulin genes, SV40, cytomegalovirus, etc.), and a polyadenylation sequence, and may include splice donor and acceptor sequences.
The plasmids can be transferred into the chosen host cell by well-known methods such as calcium chloride transformation for E. coli and calcium phosphate treatment or electroporation for mammalian cells. Cells transformed by the plasmids can be selected by resistance to antibiotics conferred by genes contained on the plasmids, such as the amp, gpt, neo and hyg genes.
Once expressed, the recombinant peptide(s) or fusion protein(s) can be purified according to standard procedures of the art, including ammonium sulfate precipitation, affinity columns, column chromatography, gel electrophoresis and the like (see, generally, R. Scopes, (1982) Protein Purification, Springer-Verlag, N.Y.; Deutscher (1990) Methods in Enzymology Vol. 182: Guide to Protein Purification, Academic Press, Inc. N.Y.). Substantially pure compositions of at least about 90 to 95% homogeneity are preferred, and 98 to 99% or more homogeneity are most preferred.
One of skill in the art would recognize that after chemical synthesis, biological expression, or purification, the peptide(s) or fusion protein(s) may possess a conformation substantially different than desired native conformation. In this case, it may be necessary to denature and reduce the peptide or fusion protein and then to cause the molecule to re-fold into the preferred conformation. Methods of reducing and denaturing proteins and inducing re-folding are well known to those of skill in the art (see, e.g., Debinski et al. (1993) J. Biol. Chem., 268: 14065-14070; Kreitman and Pastan (1993) Bioconjug. Chem., 4: 581-585; and Buchner, et al., (1992) Anal. Biochem., 205: 263-270). Debinski et al., for example, describes the denaturation and reduction of inclusion body proteins in guanidine-DTE. The protein is then refolded in a redox buffer containing oxidized glutathione and L-arginine.
One of skill would recognize that modifications can be made to the peptide(s) and/or fusion protein(s) proteins without diminishing their biological activity. Some modifications may be made to facilitate the cloning, expression, or incorporation of the targeting molecule into a fusion protein. Such modifications are well known to those of skill in the art and include, for example, a methionine added at the amino terminus to provide an initiation site, or additional amino acids (e.g., poly His) placed on either terminus to create conveniently located restriction sites or termination codons or purification sequences.
D) Joining Targeting Moieties to Effectors.
i. Chemical Conjugation.
Chimeric moieties are formed by joining one or more of the targeting moieties described herein to one or more effectors. In certain embodiments the targeting moieties are attached directly to the effector(s) via naturally occurring reactive groups or the targeting moiety and/or the effector(s) can be functionalized to provide such reactive groups.
In various embodiments the targeting moieties are attached to effector(s) via one or more linking agents. Thus, in various embodiments the targeting moieties and the effector(s) can be conjugated via a single linking agent or multiple linking agents. For example, the targeting moiety and the effector can be conjugated via a single multifunctional (e.g., bi-, tri-, or tetra-) linking agent or a pair of complementary linking agents. In another embodiment, the targeting moiety and the effector are conjugated via two, three, or more linking agents. Suitable linking agents include, but are not limited to, e.g., functional groups, affinity agents, stabilizing groups, and combinations thereof.
In certain embodiments the linking agent is or comprises a functional group. Functional groups include monofunctional linkers comprising a reactive group as well as multifunctional crosslinkers comprising two or more reactive groups capable of forming a bond with two or more different functional targets (e.g., labels, proteins, macromolecules, semiconductor nanocrystals, or substrate). In some preferred embodiments, the multifunctional crosslinkers are heterobifunctional crosslinkers comprising two or more different reactive groups.
Suitable reactive groups include, but are not limited to thiol (-SH), carboxylate (COOH), carboxyl (—COOH), carbonyl, amine (NH2), hydroxyl (—OH), aldehyde (—CHO), alcohol (ROH), ketone (R2CO), active hydrogen, ester, sulfhydryl (SH), phosphate (—PO3), or photoreactive moieties. Amine reactive groups include, but are not limited to e.g., isothiocyanates, isocyanates, acyl azides, NHS esters, sulfonyl chlorides, aldehydes and glyoxals, epoxides and oxiranes, carbonates, arylating agents, imidoesters, carbodiimides, and anhydrides. Thiol-reactive groups include, but are not limited to e.g., haloacetyl and alkyl halide derivates, maleimides, aziridines, acryloyl derivatives, arylating agents, and thiol-disulfides exchange reagents. Carboxylate reactive groups include, but are not limited to e.g., diazoalkanes and diazoacetyl compounds, such as carbonyldiimidazoles and carbodiimides. Hydroxyl reactive groups include, but are not limited to e.g., epoxides and oxiranes, carbonyldiimidazole, oxidation with periodate, N,N′-disuccinimidyl carbonate or N-hydroxylsuccimidyl chloroformate, enzymatic oxidation, alkyl halogens, and isocyanates. Aldehyde and ketone reactive groups include, but are not limited to e.g., hydrazine derivatives for schiff base formation or reduction amination. Active hydrogen reactive groups include, but are not limited to e.g., diazonium derivatives for mannich condensation and iodination reactions. Photoreactive groups include, but are not limited to e.g., aryl azides and halogenated aryl azides, benzophenones, diazo compounds, and diazirine derivatives.
Other suitable reactive groups and classes of reactions useful in forming chimeric moieties include those that are well known in the art of bioconjugate chemistry. Currently favored classes of reactions available with reactive chelates are those which proceed under relatively mild conditions. These include, but are not limited to, nucleophilic substitutions (e.g., reactions of amines and alcohols with acyl halides, active esters), electrophilic substitutions (e.g., enamine reactions), and additions to carbon-carbon and carbon-heteroatom multiple bonds (e.g., Michael reaction, Diels-Alder addition). These and other useful reactions are discussed in, for example, March (1985) Advanced Organic Chemistry, 3rd Ed., John Wiley & Sons, New York, Hermanson (1996) Bioconjugate Techniques, Academic Press, San Diego; and Feeney et al. (1982) Modification of Proteins; Advances in Chemistry Series, Vol. 198, American Chemical Society, Washington, D.C.
In certain embodiments, the linking agent comprises a chelator. For example, the chelator comprising the molecule, DOTA (DOTA=1,4,7,10-tetrakis(carboxymethyl)-1,4,7,10-tetraazacyclododecane), can readily be labeled with a radiolabel, such as Gd3+ and 64Cu, resulting in Gd3+-DOTA and 64Cu-DOTA respectively, attached to the targeting moiety. Other suitable chelates are known to those of skill in the art, for example, 1,4,7-triazacyclononane-N,N′,N″-triacetic acid (NOTA) derivatives being among the most well known (see, e.g., Lee et al. (1997) Nucl Med Biol. 24: 2225-23019).
A “linker” or “linking agent” as used herein, is a molecule that is used to join two or more molecules. In certain embodiments the linker is typically capable of forming covalent bonds to both molecule(s) (e.g., the targeting moiety and the effector). Suitable linkers are well known to those of skill in the art and include, but are not limited to, straight or branched-chain carbon linkers, heterocyclic carbon linkers, or peptide linkers. In certain embodiments the linkers can be joined to the constituent amino acids through their side groups (e.g., through a disulfide linkage to cysteine). However, in certain embodiments, the linkers will be joined to the alpha carbon amino and carboxyl groups of the terminal amino acids.
A bifunctional linker having one functional group reactive with a group on one molecule (e.g., a targeting peptide), and another group reactive on the other molecule (e.g., an antimicrobial peptide), can be used to form the desired conjugate. Alternatively, derivatization can be performed to provide functional groups. Thus, for example, procedures for the generation of free sulfhydryl groups on peptides are also known (See U.S. Pat. No. 4,659,839).
In certain embodiments the linking agent is a heterobifunctional crosslinker comprising two or more different reactive groups that form a heterocyclic ring that can interact with a peptide. For example, a heterobifunctional crosslinker such as cysteine may comprise an amine reactive group and a thiol-reactive group can interact with an aldehyde on a derivatized peptide. Additional combinations of reactive groups suitable for heterobifunctional crosslinkers include, for example, amine- and sulfhydryl reactive groups; carbonyl and sulfhydryl reactive groups; amine and photoreactive groups; sulfhydryl and photoreactive groups; carbonyl and photoreactive groups; carboxylate and photoreactive groups; and arginine and photoreactive groups. In one embodiment, the heterobifunctional crosslinker is SMCC.
Many procedures and linker molecules for attachment of various molecules to peptides or proteins are known (see, e.g., European Patent Application No. 188,256; U.S. Pat. Nos. 4,671,958, 4,659,839, 4,414,148, 4,699,784; 4,680,338; 4,569,789; and 4,589,071; and Borlinghaus et al. (1987) Cancer Res. 47: 4071-4075). Illustrative linking protocols are provided herein in Examples 2 and 3.
ii. Fusion Proteins.
In certain embodiments where the targeting moiety and effector are both peptides or both comprise peptides, the chimeric moiety can be chemically synthesized or recombinantly expressed as a fusion protein (i.e., a chimeric fusion protein).
In certain embodiments the chimeric fusion proteins are synthesized using recombinant DNA methodology. Generally this involves creating a DNA sequence that encodes the fusion protein, placing the DNA in an expression cassette under the control of a particular promoter, expressing the protein in a host, isolating the expressed protein and, if required, renaturing the protein.
DNA encoding the fusion proteins can be prepared by any suitable method, including, for example, cloning and restriction of appropriate sequences or direct chemical synthesis by methods such as the phosphotriester method of Narang et al. (1979) Meth. Enzymol. 68: 90-99; the phosphodiester method of Brown et al. (1979) Meth. Enzymol. 68: 109-151; the diethylphosphoramidite method of Beaucage et al. (1981) Tetra. Lett., 22: 1859-1862; and the solid support method of U.S. Pat. No. 4,458,066.
Chemical synthesis produces a single stranded oligonucleotide. This can be converted into double stranded DNA by hybridization with a complementary sequence or by polymerization with a DNA polymerase using the single strand as a template. One of skill would recognize that while chemical synthesis of DNA is limited to sequences of about 100 bases, longer sequences can be obtained by the ligation of shorter sequences.
Alternatively, subsequences can be cloned and the appropriate subsequences cleaved using appropriate restriction enzymes. The fragments can then be ligated to produce the desired DNA sequence.
In certain embodiments, DNA encoding fusion proteins of the present invention may be cloned using DNA amplification methods such as polymerase chain reaction (PCR). Thus, for example, the nucleic acid encoding a targeting antibody, a targeting peptide, and the like is PCR amplified, using a sense primer containing the restriction site for NdeI and an antisense primer containing the restriction site for HindIII. This produces a nucleic acid encoding the targeting sequence and having terminal restriction sites. Similarly an effector and/or effector/linker/spacer can be provided having complementary restriction sites. Ligation of sequences and insertion into a vector produces a vector encoding the fusion protein.
While the targeting moieties and effector(s) can be directly joined together, one of skill will appreciate that they can be separated by a peptide spacer/linker consisting of one or more amino acids. Generally the spacer will have no specific biological activity other than to join the proteins or to preserve some minimum distance or other spatial relationship between them. However, the constituent amino acids of the spacer may be selected to influence some property of the molecule such as the folding, net charge, or hydrophobicity.
The nucleic acid sequences encoding the fusion proteins can be expressed in a variety of host cells, including E. coli, other bacterial hosts, yeast, and various higher eukaryotic cells such as the COS, CHO and HeLa cells lines and myeloma cell lines. The recombinant protein gene will be operably linked to appropriate expression control sequences for each host. For E. coli this includes a promoter such as the T7, tip, or lambda promoters, a ribosome binding site and preferably a transcription termination signal. For eukaryotic cells, the control sequences will include a promoter and preferably an enhancer derived from immunoglobulin genes, SV40, cytomegalovirus, etc., and a polyadenylation sequence, and may include splice donor and acceptor sequences.
The plasmids can be transferred into the chosen host cell by well-known methods such as calcium chloride transformation for E. coli and calcium phosphate treatment or electroporation for mammalian cells. Cells transformed by the plasmids can be selected by resistance to antibiotics conferred by genes contained on the plasmids, such as the amp, gpt, neo and hyg genes.
Once expressed, the recombinant fusion proteins can be purified according to standard procedures of the art, including ammonium sulfate precipitation, affinity columns, column chromatography, gel electrophoresis and the like (see, generally, R. Scopes (1982) Protein Purification, Springer-Verlag, N.Y.; Deutscher (1990) Methods in Enzymology Vol. 182: Guide to Protein Purification, Academic Press, Inc. N.Y.). Substantially pure compositions of at least about 90 to 95% homogeneity are preferred, and 98 to 99% or more homogeneity are most preferred for pharmaceutical uses. Once purified, partially or to homogeneity as desired, the polypeptides may then be used therapeutically.
One of skill in the art would recognize that after chemical synthesis, biological expression, or purification, the fusion protein may possess a conformation substantially different than the native conformations of the constituent polypeptides. In this case, it may be necessary to denature and reduce the polypeptide and then to cause the polypeptide to re-fold into the preferred conformation. Methods of reducing and denaturing proteins and inducing re-folding are well known to those of skill in the art (See, Debinski et al. (1993) J. Biol. Chem., 268: 14065-14070; Kreitman and Pastan (1993) Bioconjug. Chem., 4: 581-585; and Buchner, et al. (1992) Anal. Biochem., 205: 263-270).
One of skill would recognize that modifications can be made to the fusion proteins without diminishing their biological activity. Some modifications may be made to facilitate the cloning, expression, or incorporation of the targeting molecule into a fusion protein. Such modifications are well known to those of skill in the art and include, for example, a methionine added at the amino terminus to provide an initiation site, or additional amino acids placed on either terminus to create conveniently located restriction sites or termination codons.
As indicated above, in various embodiments a peptide linker/spacer is used to join the one or more targeting moieties to one or more effector(s). In various embodiments the peptide linker is relatively short, typically less than about 10 amino acids, preferably less than about 8 amino acids and more preferably about 3 to about 5 amino acids. Suitable illustrative linkers include, but are not limited to PSGSP ((SEQ ID NO:3209), ASASA (SEQ ID NO: 3210), or GGG. In certain embodiments longer linkers such as (GGGGS)3 (SEQ ID NO:3211) can be used. Illustrative peptide linkers and other linkers are shown in Table 16.
TABLE 16
Illustrative peptide and non-peptide linkers.
Linker SEQ ID NO:
AAA
GGG
GGGG 3212
SGG
GGSGGS 3213
SAT
PYP
PSPSP 3214
ASA
ASASA 3215
PSPSP 3216
KKKK 3217
RRRR 3218
GGGGS 3219
GGGGS GGGGS 3220
GGGGS GGGGS GGGGS 3221
GGGGS GGGGS GGGGS GGGGS 3222
GGGGS GGGGS GGGGS GGGGS GGGGS 3223
GGGGS GGGGS GGGGS GGGGS GGGGS GGGGS 3224
2-nitrobenzene or O-nitrobenzyl
Nitropyridyl disulfide
Dioleoylphosphatidylethanolamine (DOPE)
S-acetylmercaptosuccinic acid
1,4,7,10-tetraazacyclododecane-1,4,7,10-tetracetic acid (DOTA)
β-glucuronide and β-glucuronide variants
Poly(alkylacrylic acid)
Benzene-based linkers (for example: 2,5-Bis(hexyloxy)-1,4-bis[2,5-
bis(hexyloxy)-4-formyl-phenylenevinylene]benzene) and like
molecules
Disulfide linkages
Poly(amidoamine) or like dendrimers linking multiple target and killing
peptides in one molecule
Carbon nanotubes
Hydrazone and hydrazone variant linkers
PEG of any chain length
Succinate, formate, acetate butyrate, other like organic acids
Aldols, alcohols, or enols
Peroxides
alkane or alkene groups of any chain length
One or more porphyrin or dye molecules containing free amide and
carboxylic acid groups
One or more DNA or RNA nucleotides, including polyamine and
polycarboxyl-containing variants
Inulin, sucrose, glucose, or other single, di or polysaccharides
Linoleic acid or other polyunsaturated fatty acids
Variants of any of the above linkers containing halogen or thiol
groups
(All amino-acid-based linkers could be L, D, combinations of L and D forms, β-form, and the like)
E) Multiple Targeting Moieties and/or Effectors.
As indicated above, in certain embodiments, the chimeric moieties described herein comprise multiple targeting moieties attached to a single effector or multiple effectors attached to a single targeting moiety, or multiple targeting moieties attached to multiple effectors.
Where the chimeric construct is a fusion protein this is easily accomplished by providing multiple domains that are targeting domains attached to one or more effector domains. FIG. 14 schematically illustrates a few, but not all, configurations. In various embodiments the multiple targeting domains and/or multiple effector domains can be attached to each other directly or can be separated by linkers (e.g., amino acid or peptide linkers as described above).
When the chimeric construct is a chemical conjugate linear or branched configurations (e.g., as illustrated in FIG. 14) are readily produced by using branched or multifunctional linkers and/or a plurality of different linkers.
F) Protecting Groups.
While the various peptides (e.g., targeting peptides, antimicrobial peptides, STAMPs) described herein may be shown with no protecting groups, in certain embodiments they can bear one, two, three, four, or more protecting groups. In various embodiments, the protecting groups can be coupled to the C- and/or N-terminus of the peptide(s) and/or to one or more internal residues comprising the peptide(s) (e.g., one or more R-groups on the constituent amino acids can be blocked). Thus, for example, in certain embodiments, any of the peptides described herein can bear, e.g., an acetyl group protecting the amino terminus and/or an amide group protecting the carboxyl terminus. One example of such a protected peptide is the 1845L6-21 STAMP having the amino acid sequence KFINGVLSQFVLERKPYPKLFKFLRKHLL* (SEQ ID NO:3225), where the asterisk indicates an amidated carboxyl terminus. Of course, this protecting group can be can be eliminated and/or substituted with another protecting group as described herein.
Without being bound by a particular theory, it was discovered that addition of a protecting group, particularly to the carboxyl and in certain embodiments the amino terminus can improve the stability and efficacy of the peptide.
A wide number of protecting groups are suitable for this purpose. Such groups include, but are not limited to acetyl, amide, and alkyl groups with acetyl and alkyl groups being particularly preferred for N-terminal protection and amide groups being preferred for carboxyl terminal protection. In certain particularly preferred embodiments, the protecting groups include, but are not limited to alkyl chains as in fatty acids, propionyl, formyl, and others. Particularly preferred carboxyl protecting groups include amides, esters, and ether-forming protecting groups. In one preferred embodiment, an acetyl group is used to protect the amino terminus and an amide group is used to protect the carboxyl terminus. These blocking groups enhance the helix-forming tendencies of the peptides. Certain particularly preferred blocking groups include alkyl groups of various lengths, e.g., groups having the formula: CH3—(CH2)n—CO— where n ranges from about 1 to about 20, preferably from about 1 to about 16 or 18, more preferably from about 3 to about 13, and most preferably from about 3 to about 10.
In certain embodiments, the protecting groups include, but are not limited to alkyl chains as in fatty acids, propionyl, formyl, and others. Particularly preferred carboxyl protecting groups include amides, esters, and ether-forming protecting groups. In one embodiment, an acetyl group is used to protect the amino terminus and/or an amino group is used to protect the carboxyl terminus (i.e., amidated carboxyl terminus). In certain embodiments blocking groups include alkyl groups of various lengths, e.g., groups having the formula: CH3—(CH2)n—CO— where n ranges from about 3 to about 20, preferably from about 3 to about 16, more preferably from about 3 to about 13, and most preferably from about 3 to about 10.
In certain embodiments, the acid group on the C-terminal can be blocked with an alcohol, aldehyde or ketone group and/or the N-terminal residue can have the natural amide group, or be blocked with an acyl, carboxylic acid, alcohol, aldehyde, or ketone group.
Other protecting groups include, but are not limited to Fmoc, t-butoxycarbonyl (t-BOC), 9-fluoreneacetyl group, 1-fluorenecarboxylic group, 9-florenecarboxylic group, 9-fluorenone-1-carboxylic group, benzyloxycarbonyl, xanthyl (Xan), trityl (Trt), 4-methyltrityl (Mtt), 4-methoxytrityl (Mmt), 4-methoxy-2,3,6-trimethyl-benzenesulphonyl (Mtr), Mesitylene-2-sulphonyl (Mts), 4,4-dimethoxybenzhydryl (Mbh), Tosyl (Tos), 2,2,5,7,8-pentamethyl chroman-6-sulphonyl (Pmc), 4-methylbenzyl (MeBzl), 4-methoxybenzyl (MeOBzl), benzyloxy (BzlO), benzyl (Bzl), benzoyl (Bz), 3-nitro-2-pyridinesulphenyl (Npys), 1-(4,4-dimentyl-2,6-diaxocyclohexylidene)ethyl (Dde), 2,6-dichlorobenzyl (2,6-DiCl-Bzl), 2-chlorobenzyloxycarbonyl (2-Cl-Z), 2-bromobenzyloxycarbonyl (2-Br-Z), Benzyloxymethyl (Bom), cyclohexyloxy (cHxO), t-butoxymethyl (Bum), t-butoxy (tBuO), t-Butyl (tBu), Acetyl (Ac), and Trifluoroacetyl (TFA).
Protecting/blocking groups are well known to those of skill as are methods of coupling such groups to the appropriate residue(s) comprising the peptides of this invention (see, e.g., Greene et al., (1991) Protective Groups in Organic Synthesis, 2nd ed., John Wiley & Sons, Inc. Somerset, N.J.). In illustrative embodiment, for example, acetylation is accomplished during the synthesis when the peptide is on the resin using acetic anhydride. Amide protection can be achieved by the selection of a proper resin for the synthesis. For example, a rink amide resin can be used. After the completion of the synthesis, the semipermanent protecting groups on acidic bifunctional amino acids such as Asp and Glu and basic amino acid Lys, hydroxyl of Tyr are all simultaneously removed. The peptides released from such a resin using acidic treatment comes out with the n-terminal protected as acetyl and the carboxyl protected as NH2 and with the simultaneous removal of all of the other protecting groups.
Where amino acid sequences are disclosed herein, amino acid sequences comprising, one or more protecting groups, e.g., as described above (or any other commercially available protecting groups for amino acids used, e.g., in boc or fmoc peptide synthesis) are also contemplated.
G) Peptide Circularization.
In certain embodiments the peptides described herein (e.g., AMPs, compound AMPs, STAMPs, etc.) are circularized/cyclized to produce cyclic peptides. Cyclic peptides, as contemplated herein, include head/tail, head/side chain, tail/side chain, and side chain/side chain cyclized peptides. In addition, peptides contemplated herein include homodet, containing only peptide bonds, and heterodet containing in addition disulfide, ester, thioester-bonds, or other bonds.
The cyclic peptides can be prepared using virtually any art-known technique for the preparation of cyclic peptides. For example, the peptides can be prepared in linear or non-cyclized form using conventional solution or solid phase peptide syntheses and cyclized using standard chemistries. Preferably, the chemistry used to cyclize the peptide will be sufficiently mild so as to avoid substantially degrading the peptide. Suitable procedures for synthesizing the peptides described herein as well as suitable chemistries for cyclizing the peptides are well known in the art.
In various embodiments cyclization can be achieved via direct coupling of the N- and C-terminus to form a peptide (or other) bond, but can also occur via the amino acid side chains. Furthermore it can be based on the use of other functional groups, including but not limited to amino, hydroxy, sulfhydryl, halogen, sulfonyl, carboxy, and thiocarboxy. These groups can be located at the amino acid side chains or be attached to their N- or C-terminus.
Accordingly, it is to be understood that the chemical linkage used to covalently cyclize the peptides of the invention need not be an amide linkage. In many instances it may be desirable to modify the N- and C-termini of the linear or non-cyclized peptide so as to provide, for example, reactive groups that may be cyclized under mild reaction conditions. Such linkages include, by way of example and not limitation amide, ester, thioester, CH2—NH, etc. Techniques and reagents for synthesizing peptides having modified termini and chemistries suitable for cyclizing such modified peptides are well-known in the art.
Alternatively, in instances where the ends of the peptide are conformationally or otherwise constrained so as to make cyclization difficult, it may be desirable to attach linkers to the N- and/or C-termini to facilitate peptide cyclization. Of course, it will be appreciated that such linkers will bear reactive groups capable of forming covalent bonds with the termini of the peptide. Suitable linkers and chemistries are well-known in the art and include those previously described.
Cyclic peptides and depsipeptides (heterodetic peptides that include ester (depside) bonds as part of their backbone) have been well characterized and show a wide spectrum of biological activity. The reduction in conformational freedom brought about by cyclization often results in higher receptor-binding affinities. Frequently in these cyclic compounds, extra conformational restrictions are also built in, such as the use of D- and N-alkylated-amino acids, α,β-dehydro amino acids or α,α-disubstituted amino acid residues.
Methods of forming disulfide linkages in peptides are well known to those of skill in the art (see, e.g., Eichler and Houghten (1997) Protein Pept. Lett. 4: 157-164).
Reference may also be made to Marlowe (1993) Biorg. Med. Chem. Lett. 3: 437-44 who describes peptide cyclization on TFA resin using trimethylsilyl (TMSE) ester as an orthogonal protecting group; Pallin and Tam (1995) J. Chem. Soc. Chem. Comm. 2021-2022) who describe the cyclization of unprotected peptides in aqueous solution by oxime formation; Algin et al. (1994) Tetrahedron Lett. 35: 9633-9636 who disclose solid-phase synthesis of head-to-tail cyclic peptides via lysine side-chain anchoring; Kates et al. (1993) Tetrahedron Lett. 34: 1549-1552 who describe the production of head-to-tail cyclic peptides by three-dimensional solid phase strategy; Tumelty et al. (1994) J. Chem. Soc. Chem. Comm. 1067-1068, who describe the synthesis of cyclic peptides from an immobilized activated intermediate, where activation of the immobilized peptide is carried out with N-protecting group intact and subsequent removal leading to cyclization; McMurray et al. (1994) Peptide Res. 7: 195-206) who disclose head-to-tail cyclization of peptides attached to insoluble supports by means of the side chains of aspartic and glutamic acid; Hruby et al. (1994) Reactive Polymers 22: 231-241) who teach an alternate method for cyclizing peptides via solid supports; and Schmidt and Langer (1997) J. Peptide Res. 49: 67-73, who disclose a method for synthesizing cyclotetrapeptides and cyclopentapeptides.
These methods of peptide cyclization are illustrative and non-limiting. Using the teaching provide herein, other cyclization methods will be available to one of skill in the art.
H) Identification/Verification of Active Peptides
The active AMPs, STAMPs and the like can be identified and/or validated using an in vitro screening assay. Indeed, in many instances the AMPs and/or STAMPS described herein will be used in vitro as preservatives, topical antimicrobial treatments, and the like. Additionally, despite certain apparent limitations of in vitro susceptibility tests, clinical data indicate that a good correlation exists between minimal inhibitory concentration (MIC) test results and in vivo efficacy of antibiotic compounds (see, e.g., Murray et al. (1994) Antimicrobial Susceptibility Testing, Poupard et al., eds., Plenum Press, New York; Knudsen et al. (1995) Antimicrob. Agents Chemother. 39(6): 1253-1258; and the like). Thus, AMPs useful for treating infections and diseases related thereto are also conveniently identified by demonstrated in vitro antimicrobial activity against specified microbial targets, e.g., as illustrated in Table 4).
Typically, the in vitro antimicrobial activity of antimicrobial agents is tested using standard NCCLS bacterial inhibition assays, or MIC tests (see, National Committee on Clinical Laboratory Standards “Performance Standards for Antimicrobial Susceptibility Testing,” NCCLS Document M100-S5 Vol. 14, No. 16, December 1994; “Methods for dilution antimicrobial susceptibility test for bacteria that grow aerobically-Third Edition,” Approved Standard M7-A3, National Committee for Clinical Standards, Villanova, Pa.).
It will be appreciated that other assays as are well known in the art or that will become apparent to those having skill in the art upon review of this disclosure may also be used to identify active AMPs. Such assays include, for example, the assay described in Lehrer et al. (1988) J. Immunol. Meth., 108: 153 and Steinberg and Lehrer, “Designer Assays for Antimicrobial Peptides: Disputing the ‘One Size Fits All’ Theory,” In: Antibacterial Peptide Protocols, Shafer, Ed., Humana Press, N.J. Generally, active peptides of the invention will exhibit MICs (as measured using the assays described in the examples) of less than about 100 μM, preferably less than about 80 or 60 μM, more preferably about 50 μM or less, about 25 μM or less, or about 15 μM or less, or about 10 μM or less.
IV. Administration and Formulations.
A) Pharmaceutical Formulations.
In certain embodiments, the antimicrobial peptides and/or the chimeric constructs (e.g., targeting moieties attached to antimicrobial peptide(s), targeting moieties attached to detectable label(s), etc.) are administered to a mammal in need thereof, to a cell, to a tissue, to a composition (e.g., a food), etc.). In various embodiments the compositions can be administered to detect and/or locate, and/or quantify the presence of particular microorganisms, microorganism populations, biofilms comprising particular microorganisms, and the like. In various embodiments the compositions can be administered to inhibit particular microorganisms, microorganism populations, biofilms comprising particular microorganisms, and the like.
These active agents (antimicrobial peptides and/or chimeric moieties) can be administered in the “native” form or, if desired, in the form of salts, esters, amides, prodrugs, derivatives, and the like, provided the salt, ester, amide, prodrug or derivative is suitable pharmacologically, i.e., effective in the present method(s). Salts, esters, amides, prodrugs and other derivatives of the active agents can be prepared using standard procedures known to those skilled in the art of synthetic organic chemistry and described, for example, by March (1992) Advanced Organic Chemistry; Reactions, Mechanisms and Structure, 4th Ed. N.Y. Wiley-Interscience.
Methods of formulating such derivatives are known to those of skill in the art. For example, the disulfide salts of a number of delivery agents are described in PCT Publication WO 2000/059863 which is incorporated herein by reference. Similarly, acid salts of therapeutic peptides, peptoids, or other mimetics, and can be prepared from the free base using conventional methodology that typically involves reaction with a suitable acid. Generally, the base form of the drug is dissolved in a polar organic solvent such as methanol or ethanol and the acid is added thereto. The resulting salt either precipitates or can be brought out of solution by addition of a less polar solvent. Suitable acids for preparing acid addition salts include, but are not limited to both organic acids, e.g., acetic acid, propionic acid, glycolic acid, pyruvic acid, oxalic acid, malic acid, malonic acid, succinic acid, maleic acid, fumaric acid, tartaric acid, citric acid, benzoic acid, cinnamic acid, mandelic acid, methanesulfonic acid, ethanesulfonic acid, p-toluenesulfonic acid, salicylic acid, and the like, as well as inorganic acids, e.g., hydrochloric acid, hydrobromic acid, sulfuric acid, nitric acid, phosphoric acid, and the like. An acid addition salt can be reconverted to the free base by treatment with a suitable base. Certain particularly preferred acid addition salts of the active agents herein include halide salts, such as may be prepared using hydrochloric or hydrobromic acids. Conversely, preparation of basic salts of the active agents of this invention are prepared in a similar manner using a pharmaceutically acceptable base such as sodium hydroxide, potassium hydroxide, ammonium hydroxide, calcium hydroxide, trimethylamine, or the like. In certain embodiments basic salts include alkali metal salts, e.g., the sodium salt, and copper salts.
For the preparation of salt forms of basic drugs, the pKa of the counterion is preferably at least about 2 pH lower than the pKa of the drug. Similarly, for the preparation of salt forms of acidic drugs, the pKa of the counterion is preferably at least about 2 pH higher than the pKa of the drug. This permists the counterion to bring the solution's pH to a level lower than the pHmax to reach the salt plateau, at which the solubility of salt prevails over the solubility of free acid or base. The generalized rule of difference in pKa units of the ionizable group in the active pharmaceutical ingredient (API) and in the acid or base is meant to make the proton transfer energetically favorable. When the pKa of the API and counterion are not significantly different, a solid complex may form but may rapidly disproportionate (i.e., break down into the individual entities of drug and counterion) in an aqueous environment.
Preferably, the counterion is a pharmaceutically acceptable counterion. Suitable anionic salt forms include, but are not limited to acetate, benzoate, benzylate, bitartrate, bromide, carbonate, chloride, citrate, edetate, edisylate, estolate, fumarate, gluceptate, gluconate, hydrobromide, hydrochloride, iodide, lactate, lactobionate, malate, maleate, mandelate, mesylate, methyl bromide, methyl sulfate, mucate, napsylate, nitrate, pamoate (embonate), phosphate and diphosphate, salicylate and disalicylate, stearate, succinate, sulfate, tartrate, tosylate, triethiodide, valerate, and the like, while suitable cationic salt forms include, but are not limited to aluminum, benzathine, calcium, ethylene diamine, lysine, magnesium, meglumine, potassium, procaine, sodium, tromethamine, zinc, and the like.
In various embodiments preparation of esters typically involves functionalization of hydroxyl and/or carboxyl groups that are present within the molecular structure of the active agent. In certain embodiments, the esters are typically acyl-substituted derivatives of free alcohol groups, i.e., moieties that are derived from carboxylic acids of the formula RCOOH where R is alky, and preferably is lower alkyl. Esters can be reconverted to the free acids, if desired, by using conventional hydrogenolysis or hydrolysis procedures.
Amides can also be prepared using techniques known to those skilled in the art or described in the pertinent literature. For example, amides may be prepared from esters, using suitable amine reactants, or they may be prepared from an anhydride or an acid chloride by reaction with ammonia or a lower alkyl amine.
In various embodiments, the active agents identified herein are useful for parenteral, topical, oral, nasal (or otherwise inhaled), rectal, or local administration, such as by aerosol or transdermally, for detection and/or quantification, and or localization, and/or prophylactic and/or therapeutic treatment of infection (e.g., microbial infection). The compositions can be administered in a variety of unit dosage forms depending upon the method of administration. Suitable unit dosage forms, include, but are not limited to powders, tablets, pills, capsules, lozenges, suppositories, patches, nasal sprays, injectibles, implantable sustained-release formulations, lipid complexes, etc.
The active agents (e.g., antimicrobial peptides and/or chimeric constructs) described herein can also be combined with a pharmaceutically acceptable carrier (excipient) to form a pharmacological composition. In certain embodiments, pharmaceutically acceptable carriers include those approved by a regulatory agency of the Federal or a state government or listed in the U.S. Pharmacopeia or other generally recognized pharmacopeia for use in/on animals, and more particularly in/on humans. A “carrier” refers to, for example, a diluent, adjuvant, excipient, auxiliary agent or vehicle with which an active agent of the present invention is administered.
Pharmaceutically acceptable carriers can contain one or more physiologically acceptable compound(s) that act, for example, to stabilize the composition or to increase or decrease the absorption of the active agent(s). Physiologically acceptable compounds can include, for example, carbohydrates, such as glucose, sucrose, or dextrans, antioxidants, such as ascorbic acid or glutathione, chelating agents, low molecular weight proteins, protection and uptake enhancers such as lipids, compositions that reduce the clearance or hydrolysis of the active agents, or excipients or other stabilizers and/or buffers.
Other physiologically acceptable compounds, particularly of use in the preparation of tablets, capsules, gel caps, and the like include, but are not limited to binders, diluent/fillers, disentegrants, lubricants, suspending agents, and the like.
In certain embodiments, to manufacture an oral dosage form (e.g., a tablet), an excipient (e.g., lactose, sucrose, starch, mannitol, etc.), an optional disintegrator (e.g. calcium carbonate, carboxymethylcellulose calcium, sodium starch glycollate, crospovidone etc.), a binder (e.g. alpha-starch, gum arabic, microcrystalline cellulose, carboxymethylcellulose, polyvinylpyrrolidone, hydroxypropylcellulose, cyclodextrin, etc.), and an optional lubricant (e.g., talc, magnesium stearate, polyethylene glycol 6000, etc.), for instance, are added to the active component or components (e.g., active peptide) and the resulting composition is compressed. Where necessary the compressed product is coated, e.g., known methods for masking the taste or for enteric dissolution or sustained release. Suitable coating materials include, but are not limited to ethyl-cellulose, hydroxymethylcellulose, polyoxyethylene glycol, cellulose acetate phthalate, hydroxypropylmethylcellulose phthalate, and Eudragit (Rohm & Haas, Germany; methacrylic-acrylic copolymer).
Other physiologically acceptable compounds include wetting agents, emulsifying agents, dispersing agents or preservatives that are particularly useful for preventing the growth or action of microorganisms. Various preservatives are well known and include, for example, phenol and ascorbic acid. One skilled in the art would appreciate that the choice of pharmaceutically acceptable carrier(s), including a physiologically acceptable compound depends, for example, on the route of administration of the active agent(s) and on the particular physio-chemical characteristics of the active agent(s).
In certain embodiments the excipients are sterile and generally free of undesirable matter. These compositions can be sterilized by conventional, well-known sterilization techniques. For various oral dosage form excipients such as tablets and capsules sterility is not required. The USP/NF standard is usually sufficient.
In certain therapeutic applications, the compositions of this invention are administered, e.g., topically administered or administered to the oral or nasal cavity, to a patient suffering from infection or at risk for infection or prophylactically to prevent dental caries or other pathologies of the teeth or oral mucosa characterized by microbial infection in an amount sufficient to prevent and/or cure and/or at least partially prevent or arrest the disease and/or its complications. An amount adequate to accomplish this is defined as a “therapeutically effective dose.” Amounts effective for this use will depend upon the severity of the disease and the general state of the patient's health. Single or multiple administrations of the compositions may be administered depending on the dosage and frequency as required and tolerated by the patient. In any event, the composition should provide a sufficient quantity of the active agents of the formulations of this invention to effectively treat (ameliorate one or more symptoms in) the patient.
The concentration of active agent(s) can vary widely, and will be selected primarily based on activity of the active ingredient(s), body weight and the like in accordance with the particular mode of administration selected and the patient's needs. Concentrations, however, will typically be selected to provide dosages ranging from about 0.1 or 1 mg/kg/day to about 50 mg/kg/day and sometimes higher. Typical dosages range from about 3 mg/kg/day to about 3.5 mg/kg/day, preferably from about 3.5 mg/kg/day to about 7.2 mg/kg/day, more preferably from about 7.2 mg/kg/day to about 11.0 mg/kg/day, and most preferably from about 11.0 mg/kg/day to about 15.0 mg/kg/day. In certain preferred embodiments, dosages range from about 10 mg/kg/day to about 50 mg/kg/day. In certain embodiments, dosages range from about 20 mg to about 50 mg given orally twice daily. It will be appreciated that such dosages may be varied to optimize a therapeutic and/or phophylactic regimen in a particular subject or group of subjects.
In certain embodiments, the active agents of this invention are administered to the oral cavity. This is readily accomplished by the use of lozenges, aersol sprays, mouthwash, coated swabs, and the like.
In certain embodiments, the active agent(s) of this invention are administered topically, e.g., to the skin surface, to a topical lesion or wound, to a surgical site, and the like.
In certain embodiments the active agents of this invention are administered systemically (e.g., orally, or as an injectable) in accordance with standard methods well known to those of skill in the art. In other preferred embodiments, the agents, can also be delivered through the skin using conventional transdermal drug delivery systems, i.e., transdermal “patches” wherein the active agent(s) are typically contained within a laminated structure that serves as a drug delivery device to be affixed to the skin. In such a structure, the drug composition is typically contained in a layer, or “reservoir,” underlying an upper backing layer. It will be appreciated that the term “reservoir” in this context refers to a quantity of “active ingredient(s)” that is ultimately available for delivery to the surface of the skin. Thus, for example, the “reservoir” may include the active ingredient(s) in an adhesive on a backing layer of the patch, or in any of a variety of different matrix formulations known to those of skill in the art. The patch may contain a single reservoir, or it may contain multiple reservoirs.
In one embodiment, the reservoir comprises a polymeric matrix of a pharmaceutically acceptable contact adhesive material that serves to affix the system to the skin during drug delivery. Examples of suitable skin contact adhesive materials include, but are not limited to, polyethylenes, polysiloxanes, polyisobutylenes, polyacrylates, polyurethanes, and the like. Alternatively, the drug-containing reservoir and skin contact adhesive are present as separate and distinct layers, with the adhesive underlying the reservoir which, in this case, may be either a polymeric matrix as described above, or it may be a liquid or hydrogel reservoir, or may take some other form. The backing layer in these laminates, which serves as the upper surface of the device, preferably functions as a primary structural element of the “patch” and provides the device with much of its flexibility. The material selected for the backing layer is preferably substantially impermeable to the active agent(s) and any other materials that are present.
Other formulations for topical delivery include, but are not limited to, ointments, gels, sprays, fluids, and creams. Ointments are semisolid preparations that are typically based on petrolatum or other petroleum derivatives. Creams containing the selected active agent are typically viscous liquid or semisolid emulsions, often either oil-in-water or water-in-oil. Cream bases are typically water-washable, and contain an oil phase, an emulsifier and an aqueous phase. The oil phase, also sometimes called the “internal” phase, is generally comprised of petrolatum and a fatty alcohol such as cetyl or stearyl alcohol; the aqueous phase usually, although not necessarily, exceeds the oil phase in volume, and generally contains a humectant. The emulsifier in a cream formulation is generally a nonionic, anionic, cationic or amphoteric surfactant. The specific ointment or cream base to be used, as will be appreciated by those skilled in the art, is one that will provide for optimum drug delivery. As with other carriers or vehicles, an ointment base should be inert, stable, nonirritating and nonsensitizing.
As indicated above, various buccal, and sublingual formulations are also contemplated.
In certain embodiments, one or more active agents of the present invention can be provided as a “concentrate”, e.g., in a storage container (e.g., in a premeasured volume) ready for dilution, or in a soluble capsule ready for addition to a volume of water, alcohol, hydrogen peroxide, or other diluent.
While the invention is described with respect to use in humans, it is also suitable for animal, e.g., veterinary use. Thus certain preferred organisms include, but are not limited to humans, non-human primates, canines, equines, felines, porcines, ungulates, largomorphs, and the like.
B) Nanoemulsion Formulations.
In certain embodiments the targeting peptides, antimicrobial peptides and/or chimeric moieties (e.g., STAMPs) as described herein are formulated in a nanoemulsion. Nanoemulsions include, but are not limited to oil in water (0/W) nanoemulsions, and water in oil (W/O) nanoemulsions. Nanoemulsions can be defined as emulsions with mean droplet diameters ranging from about 20 to about 1000 nm. Usually, the average droplet size is between about 20 nm or 50 nm and about 500 nm. The terms sub-micron emulsion (SME) and mini-emulsion are used as synonyms.
Illustrative oil in water (O/W) nanoemulsions include, but are not limited to:
Surfactant micelles—micelles composed of small molecules surfactants or detergents (e.g., SDS/PBS/2-propanol) which are suitable for predominantly hydrophobic peptides.
Polymer micelles—micelles composed of polymer, copolymer, or block copolymer surfactants (e.g., Pluronic L64/PBS/2-propanol) which are suitable for predominantly hydrophobic peptides;
Blended micelles: micelles in which there is more than one surfactant component or in which one of the liquid phases (generally an alcohol or fatty acid compound) participates in the formation of the micelle (e.g., Octanoic acid/PBS/EtOH) which are suitable for predominantly hydrophobic peptides;
Integral peptide micelles—blended micelles in which the peptide serves as an auxiliary surfactant, forming an integral part of the micelle (e.g., amphipathic peptide/PBS/mineral oil) which are suitable for amphipathic peptides; and
Pickering (solid phase) emulsions—emulsions in which the peptides are associated with the exterior of a solid nanoparticle (e.g., polystyrene nanoparticles/PBS/no oil phase) which are suitable for amphipathic peptides.
Illustrative water in oil (W/O) nanoemulsions include, but are not limited to:
Surfactant micelles—micelles composed of small molecules surfactants or detergents (e.g., dioctyl sulfosuccinate/PBS/2-propanol, Isopropylmyristate/PBS/2-propanol, etc.) which are suitable for predominantly hydrophilic peptides;
Polymer micelles—micelles composed of polymer, copolymer, or block copolymer surfactants (e.g., PLURONIC® L121/PBS/2-propanol), which are suitable for predominantly hydrophilic peptides;
Blended micelles—micelles in which there is more than one surfactant component or in which one of the liquid phases (generally an alcohol or fatty acid compound) participates in the formation of the micelle (e.g., capric/caprylic diglyceride/PBS/EtOH) which are suitable for predominantly hydrophilic peptides;
Integral peptide micelles—blended micelles in which the peptide serves as an auxiliary surfactant, forming an integral part of the micelle (e.g., amphipathic peptide/PBS/polypropylene glycol) which are suitable for amphipathic peptides; and
Pickering (solid phase) emulsions—emulsions in which the peptides are associated with the exterior of a solid nanoparticle (e.g., chitosan nanoparticles/no aqueous phase/mineral oil) which are suitable for amphipathic peptides.
As indicated above, in certain embodiments the nanoemulsions comprise one or more surfactants or detergents. In some embodiments the surfactant is a non-anionic detergent (e.g., a polysorbate surfactant, a polyoxyethylene ether, etc.). Surfactants that find use in the present invention include, but are not limited to surfactants such as the TWEEN®, TRITON®, and TYLOXAPOL® families of compounds.
In certain embodiments the emulsions further comprise one or more cationic halogen containing compounds, including but not limited to, cetylpyridinium chloride. In still further embodiments, the compositions further comprise one or more compounds that increase the interaction (“interaction enhancers”) of the composition with microorganisms (e.g., chelating agents like ethylenediaminetetraacetic acid, or ethylenebis(oxyethylenenitrilo)tetraacetic acid in a buffer).
In some embodiments, the nanoemulsion further comprises an emulsifying agent to aid in the formation of the emulsion. Emulsifying agents include compounds that aggregate at the oil/water interface to form a kind of continuous membrane that prevents direct contact between two adjacent droplets. Certain embodiments of the present invention feature oil-in-water emulsion compositions that may readily be diluted with water to a desired concentration without impairing their anti-pathogenic properties.
In addition to discrete oil droplets dispersed in an aqueous phase, certain oil-in-water emulsions can also contain other lipid structures, such as small lipid vesicles (e.g., lipid spheres that often consist of several substantially concentric lipid bilayers separated from each other by layers of aqueous phase), micelles (e.g., amphiphilic molecules in small clusters of 50-200 molecules arranged so that the polar head groups face outward toward the aqueous phase and the apolar tails are sequestered inward away from the aqueous phase), or lamellar phases (lipid dispersions in which each particle consists of parallel amphiphilic bilayers separated by thin films of water).
These lipid structures are formed as a result of hydrophobic forces that drive apolar residues (e.g., long hydrocarbon chains) away from water. The above lipid preparations can generally be described as surfactant lipid preparations (SLPs). SLPs are minimally toxic to mucous membranes and are believed to be metabolized within the small intestine (see e.g., Hamouda et al., (1998) J. Infect. Disease 180: 1939).
In certain embodiments the emulsion comprises a discontinuous oil phase distributed in an aqueous phase, a first component comprising an alcohol and/or glycerol, and a second component comprising a surfactant or a halogen-containing compound. The aqueous phase can comprise any type of aqueous phase including, but not limited to, water (e.g., dionized water, distilled water, tap water) and solutions (e.g., phosphate buffered saline solution, or other buffer systems). The oil phase can comprise any type of oil including, but not limited to, plant oils (e.g., soybean oil, avocado oil, flaxseed oil, coconut oil, cottonseed oil, squalene oil, olive oil, canola oil, corn oil, rapeseed oil, safflower oil, and sunflower oil), animal oils (e.g., fish oil), flavor oil, water insoluble vitamins, mineral oil, and motor oil. In certain embodiments, the oil phase comprises 30-90 vol % of the oil-in-water emulsion (i.e., constitutes 30-90% of the total volume of the final emulsion), more preferably 50-80%.
In certain embodiments the alcohol, when present, is ethanol.
While the present invention is not limited by the nature of the surfactant, in some preferred embodiments, the surfactant is a polysorbate surfactant (e.g., TWEEN 20®, TWEEN 40®, TWEEN 60®, and TWEEN 80®), a pheoxypolyethoxyethanol (e.g., TRITON® X-100, X-301, X-165, X-102, and X-200, and TYLOXAPOL®), or sodium dodecyl sulfate, and the like.
In certain embodiments a halogen-containing component is present. the nature of the halogen-containing compound, in some preferred embodiments the halogen-containing compound comprises a chloride salt (e.g., NaCl, KCl, etc.), a cetylpyridinium halide, a cetyltrimethylammonium halide, a cetyldimethylethylammonium halide, a cetyldimethylbenzylammonium halide, a cetyltributylphosphonium halide, dodecyltrimethylammonium halides, tetradecyltrimethylammonium halides, cetylpyridinium chloride, cetyltrimethylammonium chloride, cetylbenzyldimethylammonium chloride, cetylpyridinium bromide, cetyltrimethylammonium bromide, cetyldimethylethylammonium bromide, cetyltributylphosphonium bromide, dodecyltrimethylammonium bromide, tetradecyltrimethylammonium bromide, and the like
In certain embodiments the emulsion comprises a quaternary ammonium compound. Quaternary ammonium compounds include, but are not limited to, N-alkyldimethyl benzyl ammonium saccharinate, 1,3,5-Triazine-1,3,5(2H,4H,6H)-triethanol; 1-Decanaminium, N-decyl-N,N-dimethyl-, chloride (or) Didecyl dimethyl ammonium chloride; 2-(2-(p-(Diisobuyl)cresosxy)ethoxy)ethyl dimethyl benzyl ammonium chloride; 2-(2-(p-(Diisobutyl)phenoxy)ethoxy)ethyl dimethyl benzyl ammonium chloride; alkyl 1 or 3 benzyl-1-(2-hydroxethyl)-2-imidazolinium chloride; alkyl bis(2-hydroxyethyl)benzyl ammonium chloride; alkyl demethyl benzyl ammonium chloride; alkyl dimethyl 3,4-dichlorobenzyl ammonium chloride (100% C12); alkyl dimethyl 3,4-dichlorobenzyl ammonium chloride (50% C14, 40% C12, 10% C16); alkyl dimethyl 3,4-dichlorobenzyl ammonium chloride (55% C14, 23% C12, 20% C16); alkyl dimethyl benzyl ammonium chloride; alkyl dimethyl benzyl ammonium chloride (100% C14); alkyl dimethyl benzyl ammonium chloride (100% C16); alkyl dimethyl benzyl ammonium chloride (41% C14, 28% C12); alkyl dimethyl benzyl ammonium chloride (47% C12, 18% C14); alkyl dimethyl benzyl ammonium chloride (55% C16, 20% C14); alkyl dimethyl benzyl ammonium chloride (58% C14, 28% C16); alkyl dimethyl benzyl ammonium chloride (60% C14, 25% C12); alkyl dimethyl benzyl ammonium chloride (61% C11, 23% C14); alkyl dimethyl benzyl ammonium chloride (61% C12, 23% C14); alkyl dimethyl benzyl ammonium chloride (65% C12, 25% C14); alkyl dimethyl benzyl ammonium chloride (67% C12, 24% C14); alkyl dimethyl benzyl ammonium chloride (67% C12, 25% C14); alkyl dimethyl benzyl ammonium chloride (90% C14, 5% C12); alkyl dimethyl benzyl ammonium chloride (93% C14, 4% C12); alkyl dimethyl benzyl ammonium chloride (95% C16, 5% C18); alkyl dimethyl benzyl ammonium chloride (and) didecyl dimethyl ammonium chloride; alkyl dimethyl benzyl ammonium chloride (as in fatty acids); alkyl dimethyl benzyl ammonium chloride (C12-C16); alkyl dimethyl benzyl ammonium chloride (C12-C18); alkyl dimethyl benzyl and dialkyl dimethyl ammonium chloride; alkyl dimethyl dimethybenzyl ammonium chloride; alkyl dimethyl ethyl ammonium bromide (90% C14, 5% C16, 5% C12); alkyl dimethyl ethyl ammonium bromide (mixed alkyl and alkenyl groups as in the fatty acids of soybean oil); alkyl dimethyl ethylbenzyl ammonium chloride; alkyl dimethyl ethylbenzyl ammonium chloride (60% C14); alkyl dimethyl isoproylbenzyl ammonium chloride (50% C12, 30% C14, 17% C16, 3% C18); alkyl trimethyl ammonium chloride (58% C18, 40%
C16, 1% C14, 1% C12); alkyl trimethyl ammonium chloride (90% C18, 10% C16); alkyldimethyl(ethylbenzyl) ammonium chloride (C12-18); Di-(C8-10)-alkyl dimethyl ammonium chlorides; dialkyl dimethyl ammonium chloride; dialkyl dimethyl ammonium chloride; dialkyl dimethyl ammonium chloride; dialkyl methyl benzyl ammonium chloride; didecyl dimethyl ammonium chloride; diisodecyl dimethyl ammonium chloride; dioctyl dimethyl ammonium chloride; dodecyl bis(2-hydroxyethyl) octyl hydrogen ammonium chloride; dodecyl dimethyl benzyl ammonium chloride; dodecylcarbamoyl methyl dimethyl benzyl ammonium chloride; heptadecyl hydroxyethylimidazolinium chloride; hexahydro-1,3,5-thris(2-hydroxyethyl)-s-triazine; myristalkonium chloride (and) Quat RNIUM 14; N,N-Dimethyl-2-hydroxypropylammonium chloride polymer; n-alkyl dimethyl benzyl ammonium chloride; n-alkyl dimethyl ethylbenzyl ammonium chloride; n-tetradecyl dimethyl benzyl ammonium chloride monohydrate; octyl decyl dimethyl ammonium chloride; octyl dodecyl dimethyl ammonium chloride; octyphenoxyethoxyethyl dimethyl benzyl ammonium chloride; oxydiethylenebis (alkyl dimethyl ammonium chloride); quaternary ammonium compounds, dicoco alkyldimethyl, chloride; trimethoxysily propyl dimethyl octadecyl ammonium chloride; trimethoxysilyl quats, trimethyl dodecylbenzyl ammonium chloride; n-dodecyl dimethyl ethylbenzyl ammonium chloride; n-hexadecyl dimethyl benzyl ammonium chloride; n-tetradecyl dimethyl benzyl ammonium chloride; n-tetradecyl dimethyl ethylbenzyl ammonium chloride; and n-octadecyl dimethyl benzyl ammonium chloride.
Nanoemulsion formulations and methods of making such are well known to those of skill in the art and described for example in U.S. Pat. Nos: 7,476,393, 7,468,402, 7,314,624, 6,998,426, 6,902,737, 6,689,371, 6,541,018, 6,464,990, 6,461,625, 6,419,946, 6,413,527, 6,375,960, 6,335,022, 6,274,150, 6,120,778, 6,039,936, 5,925,341, 5,753,241, 5,698,219, an d5,152,923 and in Fanun et al. (2009) Microemulsions: Properties and Applications (Surfactant Science), CRC Press, Boca Ratan Fla.
C) Formulations Optimizing Activity.
In certain embodiments, formulations are selected to optimize binding specificity, and/or binding avidity, and/or antimicrobial activity, and/or stability/conformation of the targeting peptide, antimicrobial peptide, chimeric moiety, and/or STAMP. In this regard, it was a surprising discovery that the activity of certain STAMPs, and presumably the constituent targeting peptides and/or antimicrobial peptides was optimized in the presence of a salt. Accordingly, certain embodiments are contemplated where the targeting peptide and/or antimicrobial peptide, and/or STAMP is formulated in combination with one or more salts. The formulatiosn disclosed herein, however, are not limited to those containing salt(s). Embodiments, are also contemplated where the targeting peptide and/or antimicrobial peptide, and/or STAMP is formulated without the presence of a salt.
In certain embodiments, sodium chloride plus a little potassium chloride resulted in the best activity of the salts tested. However, other salts, e.g., CaCl2, MgCL2, MnCl2 also enhanced activity. Accordingly, in certain embodiments, it is contemplated that the targeting peptide(s), and/or antimicrobial peptide(s), and/or chimeric moieties, and/or STAMPs are formulated with one or more salts.
In certain embodiments suitable salts include any of a number of pharmaceutically acceptable salts. Representative salts include the hydrobromide, hydrochloride, sulfate, bisulfate, phosphate, nitrate, acetate, valerate, oleate, palmitate, stearate, laurate, benzoate, lactate, phosphate, tosylate, citrate, maleate, fumarate, succinate, tartrate, napthylate, mesylate, besylate, glucoheptonate, lactobionate, and laurylsulphonate salts and the like (see, e.g., Berge et al. (1977) J. Pharm. Sci. 66: 1-19), although it is noted that citrate salts appear to inhibit the activity of certain STAMPs.
In certain embodiments pharmaceutically acceptable salts of the present invention include the conventional nontoxic salts or quaternary ammonium salts of the compounds, e.g., from non-toxic organic or inorganic acids. For example, such conventional nontoxic salts include those derived from inorganic acids such as hydrochloride, hydrobromic, sulfuric, sulfamic, phosphoric, nitric, and the like; and the salts prepared from organic acids such as acetic, propionic, succinic, glycolic, stearic, lactic, malic, tartaric, citric, ascorbic, palmitic, maleic, hydroxymaleic, phenylacetic, glutamic, benzoic, salicyclic, sulfanilic, 2-acetoxybenzoic, fumaric, toluenesulfonic, methanesulfonic, benzenesulfonic, ethane disulfonic, oxalic, isothionic, and the like.
In other cases, the compounds of the present invention may contain one or more acidic functional groups and, thus, are capable of forming pharmaceutically-acceptable salts with pharmaceutically-acceptable bases. The term “pharmaceutically-acceptable salts” in these instances refers to the relatively non-toxic, inorganic and organic base addition salts of compounds of the present invention. These salts can likewise be prepared in situ in the administration vehicle or the dosage form manufacturing process, or by separately treating the compound in its free acid form with a suitable base, such as the hydroxide, carbonate or bicarbonate of a pharmaceutically-acceptable metal cation, with ammonia, or with a pharmaceutically-acceptable organic primary, secondary or tertiary amine. Representative alkali or alkaline earth salts include the lithium, sodium, potassium, calcium, magnesium, and aluminum salts and the like. Representative organic amines useful for the formation of base addition salts include ethylamine, diethylamine, ethylenediamine, ethanolamine, diethanolamine, piperazine and the like (see, for example, Berge et al., supra; and Stahl and Wermuth (2002) Handbook of Pharmaceutical Salts : Properties, Selection, and Use, Wiley-VCH, Zurich, Switzerland).
In various embodiments, the salt is simply a sodium chloride and/or a potassium chloride and can readily be prepared, for example, as a phosphate buffered saline (PBS) solution. In certain embodiments, the salt concentration is comparable to that found in 0.5× PBS to about 2.5× PBS, more preferably from about 0.5× PBS to about 1.5× PBS. In certain embodiments optimum activity has been observed in 1× PBS.
In various embodiments, the pH of the formulation ranges from about pH 5.0 to about pH 8.5, preferably from about pH 6.0 to about pH 8.0, more preferably from about pH 7.0 to about pH 8.0. In certain embodiments the pH is about pH 7.4.
While optimum results have been observed for certain STAMPs using a PBS buffer system, other buffer systems are also acceptable. Such buffers include, but are not limited to sulfate buffers, carbonate buffers, Tris buffers, CHAPS buffers, PIPES buffers, and the like, as long as the salt is included.
In various embodiments, the targeting peptide, and/or antimicrobial peptide, and/or chimeric moiety, and/or STAMP is present in the formulation at a concentration ranging from about 1 nM, to about 1, 10, or 100 mM, more preferably from about 1 nM, about 10 nM, about 100 nM, about 1 μM, or about 10 μM to about 50 μM, about 100 μM, about 200 μm, about 300 μM, about 400 μM, or about 500 μM, preferably from about 1 μM, about 10 μM, about 25 μM, or about 50 μM to about 1 mM, about 10 mM, about 20 mM, or about 5 mM, most preferably from about 10 μM, about 20 μM, or about 50 μM to about 100 μM, about 150 μM, or about 200 μM.
D) Home Health Care/Hygiene Product Formulations.
In certain embodiments, one or more of the targeting peptide(s), and/or antimicrobial peptides (AMPs) and/or chimeric moieties, and/or STAMPS described herein are incorporated into healthcare formulations, e.g., for home use. Such formulations include, but are not limited to toothpaste, mouthwash, tooth whitening strips or solutions, contact lens storage, wetting, or cleaning solutions, dental floss, toothpicks, toothbrush bristles, oral sprays, oral lozenges, nasal sprays, aerosolizers for oral and/or nasal application, wound dressings (e.g., bandages), and the like.
For example, chimeric moieties and/or STAMPs, and/or AMPs directed against S. mutans are well suited for inhibiting frequency or severity of dental caries formation, plaque formation, periodontal disease, and/or halitosis.
Chimeric moieties and/or STAMPs, and/or AMPs directed against Corynebacterium spp, when applied to a skin surface can reduce/eliminate Corynebacterium resulting in a reduction of odors. Such moieties are readily incorporated in soaps, antibiotics, antiseptics, disinfectants, and the like.
The formulation of such health products is well known to those of skill, and the antimicrobial peptides and/or chimeric constructs are simply added to such formulations in an effective dose (e.g., a prophylactic dose to inhibit dental carie formation, etc.).
For example, toothpaste formulations are well known to those of skill in the art. Typically such formulations are mixtures of abrasives and surfactants; anticaries agents, such as fluoride; tartar control ingredients, such as tetrasodium pyrophosphate and methyl vinyl ether/maleic anhydride copolymer; pH buffers; humectants, to prevent dry-out and increase the pleasant mouth feel; and binders, to provide consistency and shape (see, e.g., Table 17). Binders keep the solid phase properly suspended in the liquid phase to prevent separation of the liquid phase out of the toothpaste. They also provide body to the dentifrice, especially after extrusion from the tube onto the toothbrush.
TABLE 17
Typical components of toothpaste.
Ingredients Wt %
Humectants 40-70
Water 0-50
Buffers/salts/tartar 0.5-10
control
Organic thickeners 0.4-2
(gums)
Inorganic thickeners 0-12
Abrasives 10-50
Actives (e.g., triclosan) 0.2-1.5
Surfactants 0.5-2
Flavor and sweetener 0.8-1.5
Fluoride sources provide 1000-15000 ppm fluorine.
Table 18 lists typical ingredients used in formulations; the final combination will depend on factors such as ingredient compatibility and cost, local customs, and desired benefits and quality to be delivered in the product. It will be recognized that one or more antimicrobial peptides and/or chimeric constructs described herein can simply be added to such formulations or used in place of one or more of the other ingredients.
TABLE 18
List of typical ingredients.
Tartar
Inorganic Control
Gums Thickeners Abrasives Surfactants Humectants Ingredient
Sodium Silica Hydrated Sodium Glycerine Tetrasodium
carboxymethyl thickeners silica lauryl sulfate pyrophosphate
cellulose
Cellulose ethers Sodium Dicalcium Sodium N- Sorbitol Gantrez S-70
aluminum phosphate lauryl
silicates digydrate sarcosinate
Xanthan Gum Clays Calcium Pluronics Propylene Sodium tri-
carbonate glycol polyphosphate
Carrageenans Sodium Xylitol
bicarbonate
Sodium alginate Calcium Sodium Polyethylene
pyrophosphate lauryl glycol
sulfoacetate
Carbopols Alumina
One illustrative formulation described in U.S. Pat. No. 6,113,887 comprises (1) a water-soluble bactericide selected from the group consisting of pyridinium compounds, quaternary ammonium compounds and biguanide compounds in an amount of 0.001% to 5.0% by weight, based on the total weight of the composition; (2) a cationically-modified hydroxyethylcellulose having an average molecular weight of 1,000,000 or higher in the hydroxyethylcellulose portion thereof and having a cationization degree of 0.05 to 0.5 mol/glucose in an amount of 0.5% to 5.0% by weight, based on the total weight of the composition; (3) a surfactant selected from the group consisting of polyoxyethylene polyoxypropylene block copolymers and alkylolamide compounds in an amount of 0.5% to 13% by weight, based on the total weight of the composition; and (4) a polishing agent of the non-silica type in an amount of 5% to 50% by weight, based on the total weight of the composition. In certain embodiments, the antimicrobial peptide(s) and/or chimeric construct(s) described herein can be used in place of the bactericide or in combination with the bactericide.
Similarly, mouthwash formulations are also well known to those of skill in the art. Thus, for example, mouthwashes containing sodium fluoride are disclosed in U.S. Pat. Nos. 2,913,373, 3,975,514, and 4,548,809, and in US Patent Publications US 2003/0124068 A1, US 2007/0154410 A1, and the like. Mouthwashes containing various alkali metal compounds are also known: sodium benzoate (WO 9409752); alkali metal hypohalite (US 20020114851A1); chlorine dioxide (CN 1222345); alkali metal phosphate (US 2001/0002252 A1, US 2003/0007937 A1); hydrogen sulfate/carbonate (JP 8113519); cetylpyridium chloride(CPC) (see, e.g., U.S. Pat. No. 6,117,417, U.S. Pat. No. 5,948,390, and JP 2004051511).
Mouthwashes containing higher alcohol (see, e.g., US 2002/0064505 A1, US 2003/0175216 A1); hydrogen peroxide (see, e.g., CN 1385145); CO2 gas bubbles (see, e.g., JP 1275521 and JP 2157215) are also known. In certain embodiments, these and other mouthwash formulations can further comprise one or more of the AMPs or compound AMPs of this invention.
Contact lens storage, wetting, or cleaning solutions, dental floss, toothpicks, toothbrush bristles, oral sprays, oral lozenges, nasal sprays, and aerosolizers for oral and/or nasal application, and the like are also well known to those of skill in the art and can readily be adapted to incorporate one or more antimicrobial peptide(s) and/or chimeric construct(s) described herein.
The foregoing pharmaceutical and/or home healthcare formulations and/or devices are meant to be illustrative and not limiting. Using teaching provided herein, the antimicrobial peptide(s) and/or chimeric construct(s) described herein can readily be incorporated into other products.
E) Illustrative Oral Care Formulations.
The targeting peptide(s), and/or antimicrobial peptide(s), and/or chimeric moieties, and/or STAMPs described herein can be used for a number of applications, e.g., as described above. In certain embodiments anti-S. mutans STAMPs, AMPs, and/or other chimeric moieties can be used to reduce the incidence or severity of dental caries, inhibit plaque formation, reduce halitosis, and the like. Accordingly, in certain embodiments, such moieties are included in devices and formulations for dental applications e.g., tea or other drinks, toothpick coatings, dental floss coatings, toothpaste, gel, mouthwash, varnish, even professional dental products.
In certain embodiments, methods of treating or reducing the incidence, duration, or severity of periodontal disease are provided. The methods can include applying to the gingival crevice or periodontal pocket a composition comprising a targeting peptide, and/or antimicrobial peptide, and/or STAMP, and/or other chimeric moiety as described herein with a carrier/stabilizing agent. In the composition applied, the carrier/stabilizing agent can provide retention, tissue penetration, deposition and sustained release of the active agent (e.g., STAMP) for reducing the population of specific bacterial species within a periodontal biofilm and associated tissues. In certain embodiments, the carrier agent provides penetration and retention into the gingival crevice or periodontal pocket and associated tissues with sustained release of the active agent to enhance the reduction in population of select bacteria within the gingival tissue and dentinal tubule tissue.
In various embodiments, carrier agents can include, but are not limited to polylactide, polyglycolide, polylactide-co-glycolide, polycaprolactone, cellulosic-based polymers, ethylene glycol polymers and its copolymers, oxyethylene polymers, polyvinyl alcohol, chitosan and hyaluronan and its copolymers. In an aspect, the carrier agents include hydroxyethyl cellulose, hydroxypropyl cellulose, hydroxypropylmethyl cellulose, hydroxymethyl cellulose, polyvinyl alcohol, polyethylene glycol, polyethylene oxide, ethylene oxide-propylene oxide co-polymers, chitosan, hyaluronan and its copolymers, or combinations thereof. In another aspect, the carrier agents include hyaluronan or hyaluronic acid and copolymers including salts of hyaluronic acid, esters of hyaluronic acid, cross-linked gels of hyaluronic acid, enzymatic derivatives of hyaluronic acid, chemically modified derivatives of hyaluronic acid or combinations thereof. As used herein, hyaluronic acid broadly refers to naturally occurring, microbial and synthetic derivatives of acidic polysaccharides of various molecular weights constituted by residues of D-glucuronic acid polysaccharides and N-acetyl-D-glucosamine.
In certain embodiments, the active agent (e.g., STAMP, AMP, etc.) and the carrier agent are in the form of an admixture, in the form of a complex, covalently coupled, or a combination thereof. In certain embodiments, the carrier agent comprises a bioadhesive. Suitable bioadhesive carrier agents include, but are not limited to a cellulose based polymer and/or a dextrin. Suitable cellulose based polymers include, but are not limited to hydroxyethyl cellulose, hydroxypropyl cellulose, hydroxymethyl cellulose, or a mixture thereof. In one illustrative embodiment, the bioadhesive carrier agent includes polylactide, polyglycolide, polylactide-co-glycolide, polyethylene glycol, hyaluronan, hyaluronic acid, chitosan, or a mixture thereof. In certain embodiments the bioadhesive carrier agent can include a copolymer comprising polyethylene glycol, hyaluronan, hyaluronic acid, chitosan, or a mixture thereof
In certain embodiments, the carrier agent penetrates periodontal tissues. Suitable penetrating carrier agents include, but are not limited to hyaluronic acid, a hyaluronic acid derivative, chitosan, a chitosan derivative, or a mixture thereof. In an embodiment, the penetrating carrier agent includes a salt of hyaluronic acid, an ester of hyaluronic acid, an enzymatic derivative of hyaluronic acid, a cross-linked gel of hyaluronic acid, a chemically modified derivative of hyaluronic acid, or a mixture thereof.
V. Microorganism Detection.
As indicated above, the targeting moieties and/or STAMPs are useful in diagnostic compositions and methods to determine the presence or absence and/or to quantify the amount of one or microorganisms present in the environment, in a food stuff, in a biological sample, and the like.
For example, targeting peptide-antimicrobial peptide conjugates (e.g. Specifically targeted antimicrobial peptides (STAMPs)) can be used as diagnostic reagents. STAMPs (and other targeted antimicrobial constructs described herein) have the ability to specifically bind to microorganisms, for example, S. mutans, and permeabilize or disrupt their membrane such that cell impermeable dyes or other reagent (propidium iodide, etc.) may enter the microorganism or intracellular molecules or contents (ATP, DNA, Calcium, etc.) of the targeted microorganism are caused to be released into the environment for analysis. In one method a STAMP, for example, C16G2, can permeabilize or disrupt the membrane of target microorganisms, for example, S. mutans, in a prepared culture or clinical sample by itself, in a biofilm in vitro or in vivo. To the sample a cell impermeable dye (e.g. propidium iodide, etc.) is added to label and allow for detection of those microorganisms targeted by the STAMP. Cell permeable dyes (e.g. SYTO9) can also be added to label and detect the entire population of microorganisms in the sample. Labeled cells can then be quantified by fluorescence microscopy, fluorometry, flow cytometry or other method.
In another example, a STAMP treated sample is mixed with luciferase and luciferin which reacts with the ATP released from the STAMP treated cells and the resulting luminescence is used to detected and quantify targeted cells.
VI. Kits.
In another embodiment this invention provides kits for the inhibition of an infection and/or for the treatment and/or prevention of dental caries in a mammal. The kits typically comprise a container containing one or more of the active agents (i.e., the antimicrobial peptide(s) and/or chimeric construct(s)) described herein. In certain embodiments the active agent(s) can be provided in a unit dosage formulation (e.g., suppository, tablet, caplet, patch, etc.) and/or may be optionally combined with one or more pharmaceutically acceptable excipients.
In certain embodiments the kits comprise one or more of the home healthcare product formulations described herein (e.g., toothpaste, mouthwash, tooth whitening strips or solutions, contact lens storage, wetting, or cleaning solutions, dental floss, toothpicks, toothbrush bristles, oral sprays, oral lozenges, nasal sprays, aerosolizers for oral and/or nasal application, and the like).
In certain embodiments kits are provided for detecting and/or locating and/or quantifying certain target microorganisms and/or cells or tissues comprising certain target microorganisms, and/or prosthesis bearing certain target microorganisms, and/or biofilms comprising certain target microorganisms. In various embodiments these kits typically comprise a chimeric moiety comprising a targeting moiety and a detectable label as described herein and/or a targeting moiety attached to an affinity tag for use in a pretargeting strategy as described herein.
In addition, the kits optionally include labeling and/or instructional materials providing directions (i.e., protocols) for the practice of the methods or use of the “therapeutics” or “prophylactics” or detection reagents of this invention. Certain instructional materials describe the use of one or more active agent(s) of this invention to therapeutically or prophylactically to inhibit or prevent infection and/or to inhibit the formation of dental caries. The instructional materials may also, optionally, teach preferred dosages/therapeutic regiment, counter indications and the like.
While the instructional materials typically comprise written or printed materials they are not limited to such. Any medium capable of storing such instructions and communicating them to an end user is contemplated by this invention. Such media include, but are not limited to electronic storage media (e.g., magnetic discs, tapes, cartridges, chips), optical media (e.g., CD ROM), and the like. Such media may include addresses to internet sites that provide such instructional materials.
EXAMPLES The following examples are offered to illustrate, but not to limit the claimed invention.
Example 1 Design and Activity of a “Dual-Targeted” Antimicrobial Peptide Numerous reports have indicated the important role of human normal flora in the prevention of microbial pathogenesis and disease. Evidence suggests that infections at mucosal surfaces result from the outgrowth of subpopulations or clusters within a microbial community, and are not linked to one pathogenic organism alone. In order to preserve the protective normal flora while treating the majority of infective bacteria in the community, a tunable therapeutic is necessary that can discriminate between benign bystanders and multiple pathogenic organisms. Here we describe the proof-of-principle for such a multi-targeted antimicrobial: a multiple-headed specifically-targeted antimicrobial peptide (MH-STAMP). The completed MH-STAMP, M8(KH)-20, displays specific activity against targeted organisms in vitro (Pseudomonas aeruginosa and Streptococcus mutans) and can remove both species from a mixed planktonic culture with little impact against untargeted bacteria. These results demonstrate that a functional, dual-targeted molecule can be constructed from wide-spectrum antimicrobial peptide precursor.
Introduction For nearly 30 years antimicrobial peptides (AMPs) have been rigorously investigated as alternatives to small molecule antibiotics and potential solutions to the growing crisis of antibiotic resistant bacterial infections (Ganz (2003) Nat Rev Immunol., 3: 710-720; Hancock and Lehrer (1998), 16: 82-88). Numerous reports have characterized potential AMPs from natural sources, and a great body of work has been carried out designing “tailor-made” AMPs due to the approachable nature of solid-phase peptide synthesis (SPPS) (Genco et al. (2003) Int J Antimicrob Agents, 21: 75-78; He and Eckert (2007) Antimicrob Agents Chemother., 51: 1351-1358). Several examples of the latter have shown remarkable activities in vitro against fungi, Gram-positive and Gram-negative bacteria, as well as some enveloped viruses (Brogden (2005) Nat Rev Microbiol. 3: 238-250).
Unlike small molecule antibiotics that may lose activity when their basic structures are modified even incrementally, peptides are a convenient canvas for molecular alteration. AMPs can be optimized through the incorporation of more or less hydrophobic or charged amino acids, which has been shown to affect selectivity for Gram-positive, Gram-negative or fungal membranes (Muhle and Tam JP (2001) Biochemistry, 40: 5777-5785; Tossi et al. (2000) Biopolymers 55: 4-30). Additionally, lysine residues can be utilized to improve AMP activity per μM. In this approach, multiple AMP chains can be attached to a single peptide scaffold through branching from lysine epsilon-amines (Tam et al. (2992) Eur. J. Biochem., 269: 923-932; Pini et al. (2005) Antimicrob Agents Chemother., 2005;49: 2665-2672). AMP activity can be specifically tuned through the attachment of a targeting peptide region, as described for a novel class of molecules, the specifically-targeted antimicrobial peptides, or STAMPs (Eckert et al. (2006) Antimicrob Agents Chemother., 50: 3651-3657; Eckert et al. (2006) Antimicrob Agents Chemother., 50: 1480-1488). These chimeric molecules can consist of functionally independent targeting and killing moieties within a linear peptide sequence. A pathogenic bacterium recognized (i.e. bound) by the targeting peptide can be eliminated from a multi-species community with little impact to bystander normal flora. As an extension of this concept, we hypothesized that a STAMP could be constructed with multiple targeting peptide “heads” attached to a single AMP by utilizing a central lysine residue branch point. Potentially, targeting “heads” could be specific for the same pathogen, or have different binding profiles. Utilizing the former approach, microbial resistance evolution linked to a targeting peptide could be inhibited or reduced, as no single microbial population would have the genetic diversity necessary to mutate multiple discrete targeting peptide receptors in one cell (Drake et al. (1998) Genetics 148: 1667-1686).
Multi-headed STAMP (MH-STAMP) molecules with differing bacterial targets may have appeal in treating poly-microbial infections, or where it may be advantageous to remove a cluster of biofilm constituents without utilizing several distinct molecules; for example in the simultaneously treatment of dental caries and periodontitis, or in the eradication of the Propionibacteria spp. and Staphylococcus spp. involved in acne and skin infections, respectively.
In this example, we present the proof-of-principle design, synthesis and in vitro activity of such a MH-STAMP, M8(KH)-20. Previously, we identified two functional STAMP targeting domains, one with specific recognition of the cariogenic pathogen S. mutans (Eckert et al. (2006) Antimicrob Agents Chemother., 50: 3651-3657), and the other with Pseudomonas spp.-level selectivity (Eckert et al. (2006) Antimicrob Agents Chemother., 50: 3833-3838). Conjoined to a normally wide-spectrum linear AMP, we observed antimicrobial effects directed specifically to P. aeruginosa and S. mutans in vitro. Additionally, treatment of mixed bacterial communities with the multi-headed MH-STAMP resulted in the specific eradication of the target organisms with little impact on bystander population levels.
Materials and Methods Bacterial Strains and Growth Conditions
P. aeruginosa ATCC 15692, Klebsiella pneumoniae KAY 2026 (Sprenger and Lengeler (1984) J Bacteriol., 157: 39-45), Escherichia coli DH5α (pFW5, spectinomycin resistance) (Podbielski et al. (1996) Gene, 177: 137-147), Staphylococcus aureus Newmann (Duthie and Lorenz (1952) J Gen Microbiol., 6: 95-107), and Staphylococcus epidermidis ATCC 35984 were cultivated under aerobic conditions at 37° C. with vigorous shaking. Aerobic Gram-negative organisms were grown in Lauri-Bertaini (LB) broth and Gram-positive bacteria in Brain-heart infusion (BHI) broth. Streptococcus mutans JM11 (spectinomycin resistant, UA140 background) was grown in Todd-Hewitt (TH) broth under anaerobic conditions (80% N2, 15% CO2, 5% H2) at 37° C. Merritt et al. (2005) J Microbiol Meth., 61: 161-170. All bacteria were grown overnight to an OD600 of 0.8-1.0 prior to appropriate dilution and antimicrobial testing.
Synthesis of Multi-Head STAMP Peptides
Conventional solid-phase peptide synthesis (SPPS) methodologies were utilized for the construction of all peptides shown in FIG. 15 (Symphony Synthesizer, PTI, Tucson, Ariz.). Chemicals, amino acids, and synthesis resins were purchased from Anaspec (San Jose, Calif.). BD2.20 (FIRKFLKKWLL (SEQ ID NO:3226), amidated c-terminus, mw 1491.92), an antimicrobial peptide developed in our laboratory with robust antimicrobial activity against a number of bacterial species (Table 19), served as the root sequence to which differing targeting peptides were attached: Firstly, BD2.20 was synthesized by SPPS (Rink-Amide-MBHA resin, 0.015 mmol), followed by the stepwise coupling of a functionalized alkane (NH2(CH2)7COOH), and an Fmoc-protected Lys (side-chain protected with 4-methyltrityl (Mtt)) to the N-terminus. Standard SPPS methods were then employed for the step-wise addition of the S. mutans targeting peptide M8 plus a tri-Gly linker region (TFFRFLNR-GGG (SEQ ID NO:3227)) to the N-terminal of the central Lys. After assembly of Fmoc-M8-GGG-K(Mtt)-(CH2)7CO-BD2.20 (SEQ ID NO:3228), the Fmoc group was removed with 25% piperidine in DMF and the N-terminal was re-protected with an acetyl group with Ac2O/DIEA (1:1, 20 molar excess) for 2 hours. The Mtt-protected amino group of the central Lys was then selectively exposed with 2% TFA in DCM (1.5 mL) for 15 minutes (three cycles of 5 min). The resulting product was reloaded into the synthesizer and the peptide sequence built from the Lys side-chain was completed with standard Fmoc SPPS methods. As shown in FIG. 15, the completed MH-STAMP M8(KH)-20 contained the side-chain peptide KH (Pseudomonas spp.-targeting, KKHRKHRKHRKH-GGG (SEQ ID NO:3229)), while in MH-STAMP M8(BL)-20 a peptide with no bacterial binding (data not shown), BL-1 (DAANEA-GGG), was utilized. BL(KH)-20 was constructed identically to M8(KH)-20, utilizing BL-1 in place of M8 (FIG. 15).
TABLE 19
MICs of MH-STAMPs and component peptides.
MIC (μM)
P. aeruginosa E. coli K. pneumoniae S. mutans S. epidermidis S. aureus
BD2.20 14.4 ± 4.40 5.47 ± 1.41 2.98 ± 0.47 2.86 ± 0.60 5.11 ± 1.58 5.625 ± 1.29
M8(KH)- 11.95 ± 3.32 2.72 ± 0.59 3.13 6.25 3.13 5.64 ± 1.07
20
M8(BL)- 50 5.97 ± 0.94 6.88 ± 1.98 6.25 6.25 18.05 ± 6.58
20
BL(KH)- 27.5 ± 7.90 6.25 6.25 6.25 6.25 6.25
20
Average MIC with standard deviation, n = 10 assays.
Synthesis progression was monitored by the ninhydrin test, and completed peptides cleaved from the resin with 95% TFA utilizing appropriate scavengers, and precipitated in methyl tert-butyl ether. Purification and MH-STAMP quality was confirmed by HPLC (Waters, Milford, Mass.) using a linear gradient of increasing mobile phase (acetonitrile 10 to 90% in water with 0.1% TFA) and a Waters XBridge BEH 130 C18 column (4.6×100 mm, particle size 5 μm). Absorbance at 215 nm was utilized as the monitoring wavelength, though 260 and 280 nm were also collected. LC spectra were analyzed with MassLynx Software v.4.1 (Waters). Matrix-assisted laser desorption ionization (MALDI) mass spectroscopy was utilized to confirm correct peptide mass (Voyager System 4291, Applied Biosystems) (Anderson et al. (2008) Biotechnol Lett., 30: 813-818).
MIC Assay
Peptides were evaluated for basic antimicrobial activity by broth microdilution, as described previously (Eckert et al. (2006) Antimicrob Agents Chemother., 50: 3651-3657; Eckert et al. (2006) Antimicrob Agents Chemother., 50: 1480-1488). Briefly, ˜1×105 cfu/mL bacteria were diluted in TH (S. mutans), or Mueller-Hinton (MH) broth (all other organisms) and distributed to 96-well plates. Serially-diluted (2-fold) peptides were then added and the plates incubated at 37° C. for 18-24 h. Peptide MIC was determined as the concentration of peptide that completely inhibited organism growth when examined by eye (clear well). All experiments were conducted 10 times.
Post-Antibiotic Effect Assay
The activity and selectivity of MH-STAMPs after a 10 min incubation was determined by growth retardation experiments against targeted and untargeted bacteria in monocultures, as described previously (Id.). Cells from overnight cultures were diluted to ˜5×106 cfu/mL in MH (or TH with 1% sucrose for S. mutans), normalized by OD600 0.05-0.1 and seeded to 96-well plates. Cultures were then grown under the appropriate conditions for 2 h (3 h for S. mutans) prior to the addition of peptides for 10 min. Plates were then centrifuged at 3000×g for 5 min, the supernatants discarded, fresh medium returned (MH or TH without sucrose for S. mutans), and incubation resumed. Bacterial growth after treatment was then monitored over time by OD600.
Microbial Population Shift Assay
Mixed planktonic populations of P. aeruginosa, E. coli, S. epidermidis, and S. mutans were utilized to examine the potential of MH-STAMPs to direct species composition within a culture after treatment. Samples were prepared containing: ˜6×104 cfu/mL S. mutans, ˜2×104 cfu/mL E. coli, ˜2×104 cfu/mL S. epidermidis, and ˜0.5×104 cfu/mL P. aeruginosa in BHI (mixed immediately before peptide addition). Peptide (10 μM) or mock-treatment (1× PBS) was then added and samples were incubated at 37° C. for 24 h under anaerobic conditions (80% N2, 15% CO2, 5% H2). After incubation, samples were serially diluted (1:10) in 1× PBS and aliquots from each dilution were then spotted to agar plates selective for each species in the mixture: TH plus 800 μg/mL spectinomycin (S. mutans), LB plus 25 μg/mL ampicillin (P. aeruginosa), LB plus 200 μg/mL spectinomycin (E. coli), and mannitol salt agar (MSA, S. epidermidis) in order to quantitate survivors from each species. Plates were then incubated 37° C. under aerobic conditions (TH plates were incubated anaerobically) and colonies counted after 24 h to determine survivors. Expected colony morphologies were observed for each species when plated on selective media. Gram stains and direct microscopic observation (from select isolated colonies) were undertaken to confirm species identity (data not shown). The detection limit of the assay was 200 cfu/mL.
Results Design and Synthesis of Multi-Headed STAMPs
We constructed a prototype MH-STAMP from the well-established targeting peptides KH (specific to Pseudomonas spp) and M8 (specific for Streptococcus mutans). The wide-spectrum antimicrobial peptide BD2.20 was utilized as the base AMP for all MH171 STAMP construction. BD2.20 is a novel synthetic AMP with a cationic and amphipathic residue arrangement, which has robust MICs against a variety of Gram-negative and Gram-positive organisms (Table 19). For the synthesis of MH-STMAP M8(KH)-20 (construct presented in FIG. 15), BD2.20 and a Lys (Mtt-protected side-chain) residue were joined via an activated alkane spacer, followed by addition of the M8 targeting peptide to the N-terminus of the product. Selective deprotection of the central Lys(Mtt) side chain was then undertaken and the KH targeting peptide attached. The correct molecular mass (4888.79) and ˜90% purity was confirmed by HPLC and MALDI mass spectrometry (FIG. 16).
The non-binding “blank” targeting peptide BL-1 was incorporated into the synthesis scheme in place of KH or M8 to construct variant MH-STAMPs possessing a single functional targeting head: M8(BL)-20 and BL(KH)-20. The correct MW and acceptable purity were observed for these MH-STAMPs (FIG. 15, data not shown).
General Antimicrobial Activity of Multi-Head Constructs
After synthesis, the completed MH-STAMPs were evaluated for general antimicrobial activity by MIC against a panel of bacteria. As shown in Table 19, the MH-STAMP constructs M8(KH)-20, BL(KH)-20, and M8(BL)-20 were found to have similar activity profiles to that of BD2.20 for the organisms examined (less than two titration steps in 10-fold difference). Additionally, we observed a difference in general susceptibility between P. aeruginosa and the other organisms tested, suggesting this bacterium is more resistant to BD2.20. Overall, these data indicate that the addition of the targeting domains to the base sequence was tolerated and did not completely inhibit the activity of the antimicrobial peptide.
Peptide selectivity could not be determined utilizing these methods, as STAMPs and their parent AMP molecules often display similar MICs, but have radically different antimicrobial kinetics and selectivity due to increased specific-killing mediated by the targeting regions (Id.). Therefore, we performed different experiments to test for antimicrobial selectivity and functional MH-STAMP construction.
Selectivity and Post-Antibiotic Effect of MH-STAMP Constructs
MH-STAMP antimicrobial kinetics was ascertained utilizing a variation of the classical post-antibiotic effect assay, which measures the ability of an agent to affect an organism's growth after a short exposure period. Monocultures of MH-STAMP-targeted and untargeted organisms were exposed to M8(KH)-20, M8(BL)-20, BL(KH)-20, or unmodified BD2.20, then allowed to recover. As shown in FIG. 17A, S. mutans growth was effectively retarded by M8-containing constructs (M8(KH)-20, M8(BL)-20), but was not altered by a MH-STAMP construct lacking this region (BL(KH)-20). Similarly, the growth of the other targeted bacterium, P. aeruginosa, was inhibited in a KH-dependant manner (FIG. 17B). In comparison, the non-targeted bacteria E. coli, S. aureus, and S. epidermidis were not inhibited by treatment with any MH-STAMP and were only inhibited by the base antimicrobial peptide BD2.20, which displayed robust antimicrobial activity against all examined strains. These results indicate that MH-STAMPs containing KH or M8 targeting domains have activity against P. aeruginosa or S. mutans, respectively, and not other bacteria. Furthermore, replacement of the targeting region with a non-binding peptide abolishes specific activity.
Ability of MH-STAMPs to Direct a “Population Shift” Within a Mixed Species Population
We hypothesized that potential MH-STAMP dual-functionality could affect a particular set of bacteria within a mixed population, thereby promoting the outgrowth of non-targeted organisms and “shifting” the constituent makeup. To examine this possibility, defined mixed populations of planktonic cells were treated continuously and the make-up of the community examined after 24 h. As shown in FIG. 18, treatment with the wide spectrum AMP BD2.20 resulted in a significant loss of recoverable cfu/mL after 24 h from all species in the mixture. Treatment with M8(KH)-20 was found to alter this pattern; we observed ˜1×105 cfu/mL surviving E. coli and S. epidermidis, but did not recover S. mutans or P. aeruginosa cfu/mL. In BL(KH)-20 treated samples, P. aeruginosa cfu/mL were not observed, though we recovered higher than input cfu/mL from S. mutans and unchanged numbers of S. epidermidis and E. coli. In samples exposed to M8(BL)-20, S. mutans recoverable cfu/mL were greatly reduced compared to input cfu/mL, while other species were not affected or affected to a lesser extent. Interestingly, these results suggest that M8(KH)-20, M8(BL)-20, and BL(KH)-20 retain their ability to affect organisms recognized by the targeting regions present, even within a mixed population of bacteria.
Discussion Our results indicate that we have successfully constructed a STAMP with dual antimicrobial specificities controlled by the targeting peptides present in the molecule; KH for Pseudomonas spp, M8 for S. mutans. In a closed multi-species system (FIG. 18), the dual specificity of M8(KH)-20 was readily discernable: the population of the culture “shifted” away from targeted organisms after MH-STAMP treatment. The targeted bacteria were eliminated and the population of untargeted organisms increased, to varying degrees, above-input cfu/mL. Additionally, interruption of KH or M8 in the MH-STAMP construct with the non-binding peptide BL-1 resulted in the expected elimination of only one targeted species. These results support the hypothesis that functional MH-STAMPs could be constructed from a wide-spectrum AMP base.
The emergence of metagenomics and the development of more sensitive molecular diagnostics has driven an increase in the understanding of human-associated microbial ecologies and host-microbe interactions (Aas et al. (2005) J Clin Microbiol., 43: 5721-5732; Boman (2000) Immunol Rev., 173: 5-16; Kreth et al. (2005) J Bacteriol., 187: 7193-7203). At mucosal surfaces, it has become clear that our bodies harbor an abundance of residential flora which may impact innate and humoral immunity, nutrient availability, protection against pathogens, and even host physiology (Metges (2000) J Nutr., 130: 1857S-64; Sears (2005) Anaerobe, 11: 247-251; Lievin-Le et al. (2006) Clin Microbiol Rev., 19: 315-337; DiBaise et al. (2008) Mayo Clinic Proceedings 83: 460-469). Furthermore, findings have indicated that shifts in the diversity of normal flora are associated with negative clinical consequences; for example the overgrowth of S. mutans in the oral cavity during cariogenesis (linked to the uptake of sucrose) or the antibiotic-assisted colonization of the intestine by Clostridium difficle (Loesche (1986) Microbiol Rev., 50: 353-380; Gould and McDonald (2998) Crit Care 12: 203). Other population shifts may be linked to axilla odor (Corynebacteria spp) (Leyden et al. (1981) J Invest Dermatol., 77: 413-416; Elsner (2006) Curr Probl Dermatol., 33: 35-41), or even host obesity. Given the quantity and diversity of microbes present, pathogenesis at mucosal surfaces is not likely to be associated with the overgrowth of a single strain or species. More often, it is a population shift resulting in the predominance of two or more species; for example the persistence of Burkholderia cepacia and P. aeruginosa in cystic fibrosis airway or Treponema denticola and Porphymonas gingivalis and other “red cluster” organisms in gingivitis (Govan and Deretic (1996) Microbiol Rev., 60: 539-574; Paster et al. (2001) J Bacteriol., 183: 3770-3783). In many cases (such as the latter) these species may have only distant phylogenetic relationships and display differential susceptibilities to antibiotic therapies resulting in persistent disease progression despite treatment (Schlessinger (1988) Clin Microbiol Rev., 1: 54-59; Tresse et al. (1997) J Antimicrob Chemother., 40: 419-421). Currently, available treatments for infections of mucosal surfaces are largely non-specific (traditional small-molecule antibiotics, mechanical removal), and thus are not effective in retaining flora or shifting the constituent balance back to a health-associated composition (Keene and Shklair (1974) J Dent Res., 53: 1295). There is a need for a therapeutic treatment that can selectively target multiple pathogens, regardless of their phylogenetic relationship, and MH-STAMPs can help achieve this goal.
In monoculture experiments (FIG. 17), our results suggest that M8 or KH inclusion in the MH-STAMP drove activity towards S. mutans or P. aeruginosa, but also that the presence of a targeting domain reduced the activity of the parent AMP BD2.20 against untargeted organisms. In contrast, the results of our MIC assays (Table 19) indicate little difference in activity between BD2.20 and any MH-STAMP. Against untargeted organisms, the M8 and KH regions are likely to have a negative, but not completely inhibitory, impact on BD2.20 activity. Given the long duration of activity and the lower inoculum size in the MIC assay (compared with experiments in FIG. 17), it is likely that all BD2.20-containing peptides could reach equal levels of growth inhibition, despite large and target-specific differences in antimicrobial speed. This pattern of results was also observed when comparing MICs of targeted and untargeted organisms utilizing STAMPs against S. mutans and Pseudomonas mendocina (Eckert et al. (2006) Antimicrob Agents Chemother., 50: 3651-3657; Eckert et al. (2006) Antimicrob Agents Chemother., 50: 1480-1488).
Although more rigorous studies and a more medically relevant combination of pathogen targets is desirable, these findings indicate that it is possible to design an antimicrobial peptide-based therapeutic with multiple and defined fidelities in vitro. MH-STAMPs may help improve human health through the promotion of healthy microbial constituencies.
Example 2 Synthesis of Peptide-Porphyrin Conjugate: The mixture of coupling reagent HATU (5 eq. excess, 10 mg) and purpurin-18 (MW 564, 5 eq excess, 15 mg) in 600 mL dry dichloromethane (DCM):DMF:dimethylsulphoxide (DMSO) (1:1:1 (v/v)) was added to the peptide resin (1 molar equivalent, 15 mg) which was swelled by placing in minimal DMF for 30 min prior to reaction. 26 μL (10 molar equivalents) DIPEA was then added to the reaction flask to initiate the reaction. The reaction mixture was protected with argon and stirred at room temperature for 3 h.
After finishing, the reaction mixture was then passed down a sintered glass filtered vial and extensively washed with DMF and DCM to remove all waste reagents. The resin was then dried overnight in vacuum, and cleaved with 1 ml of trifluoroacetic acid (TFA)/thioanisole/water/EDT (10/0.5/0.5/025) for 2 hr at room temperature, and the cleavage solution was precipitated with 10 mL methyl-tert butyl ether. The precipitate was washed twice with the same amount of ether.
Example 3 Synthesis of Peptide-CSA Conjugate: To the fully protected peptide (solution of B43-GGG (FIDSFIRSF-GGG, 0.025 mmol) and tri-Boc-CSA-15 (0.0125 mol) in 300 μL DMF, DCC (7.7 mg), HOBt (5.1 mg) and 13 μL DIEA were added in iced-bath. After stirred at room temperature for four days, the reaction mixture was poured into 5 ml water and extracted with chloroform (5×3 mL). The CHCl3 extract was evaporated under vacuum and dried in a lyophilizer overnight. The dried CHCl3 extracts was then dissolved in 1 mL DCM followed by added 1 mL of TFA in iced-bath. The reaction mixture was further stirred at room temperature for 2 hours and precipitated with methyl tert-butyl ether (10 mL). The precipitate was further washed once with the same amount ether and dried in vacuum.
Example 4 STAMPs Against Corynebacterium jeikeium and Streptococcus mutans This example illustrates the development of STAMPs to selectively target and reduce or eliminate Streptococcus mutans (dental caries) or Corynebacterium jeikeium (body odor, opportunistic infections) from mixed microbial populations.
Axilla odor is caused by overgrowth of, and metabolite production from, Corynebacterium spp, which replaces Staphylococcus and Micrococcus spp associated with less odor. Current hygiene (soaps, antibiotics, antiseptics, disinfectants) practices remove all bacteria, allowing the ratio of Corynebacteria to normal flora to remain high during regrowth. Deodorants and anti-perspirants are temporary solutions that hide or even exacerbate the problem.
S. mutans is the major etiological agent of dental caries. Current methods (tooth brushing, antiseptic mouthrinses) to treat cariogenesis have focused on complete bacterial removal, i.e., elimination of S. mutans and other harmless oral bacteria. Caries have persisted despite these methods, and in many cases, S. mutans can become the dominant organism in the mouth. Several S. mutans and acid-targeted approaches (probiotic replacement, saliva pH adjustment) are under development, but none have shown clinical efficacy.
This example describes a number of STAMPs that preferentially or selectively reduce or eliminate S mutans and/or Corynebacterium spp from mixed populations.
Several lead STAMPs with specific activity against Corynebacterium jeikeium are also disclosed herein.
The STAMPs described herein comprise functional regions within a peptide molecule or a chemical conjugate. These regions include a targeting region comprising one or more targeting moieties (e.g., targeting peptides), a linker, and one or more killing moieties (e.g., antimicrobial peptides (AMPs), porphyrins, etc.).
The STAMPs function through the targeting region, which selectively accumulates STAMPs, and therefore killing regions, on or in proximity to the microorganism of interest. Other flora are not recognized by the targeting region, and therefore avoid or have reduced STAMP accumulation and cellular damage.
In certain embodiments, STAMPs against oral S. mutans are best applied formulated in a mouthrinse, toothpaste, cream, gel, or adhesive strip, and in certain preferably embodiments, are provided in a formulation that comprises 0.5 to 2.5× PBS (or other salt) and other ingredients commonly found in oral healthcare formulations (e.g., mouthrinse formulations). Certain illustrative formulations are shown in Table 20.
During the course of evaluating STAMPs, antimicrobial peptides (AMPs), and binding peptides for desired activity, it was discovered that certain formulations can attenuate or promote peptide activity, as compared to activity levels in a default buffer system (1× PBS). In some cases, 1× PBS may provide the best level of activity. Below are a number of formulations that alter, or may alter, peptide or STAMP activity. For complex buffer systems, assume the base solvent is water unless otherwise stated.
Formulation 1 (1× PBS, pH 7.4): 136.8 mM NaC1, 2.68 mM KC1, 1.01 mM Na2HPO4, and 1.37 mM KH2PO4.
Formulation 2 (HEPES/CTAB): 20 mM HEPES (4-(2-hydroxyethyl)-1-piperazineethanesulfonic acid), 150 mM NaC1, 1 mM MgCl2, and 0.1% CTAB (Cetyl trimethylammonium bromide).
Formulation 3 (TRIS/CTAB): 20 mM Tris (tris(hydroxymethyl)aminomethane), pH 7.5, 150 mM NaCl, 1 mM MgCl2, and 0.1% CTAB.
Formulation 4: 20 mM HEPES.
Formulation 5: 20 mM Tris, pH 7.5.
Formulation 6: 0.2% CTAB.
Formulation 7: 1% Glycerol.
Formulation 8: 1% Pluronic F108 (nonionic surfactant: α-Hydro-.omega.-hydroxypoly(oxyethylene)poly(oxypropylene)poly(oxyethylene) block copolymer).
Formulation 9: 1% Pluronic F123 (Poly(ethylene glycol)-block-poly(propylene glycol)-block-poly(ethylene glycol), average Mn ˜5,800).
Formulation 10: 1% Pluronic F17R4 (Poly(propylene glycol)-block-poly(ethylene glycol)-block-polypropylene glycol), average Mn ˜2,700).
Formulation 11: 1% to 7% PEG400.
Formulation 12: 50 mM Urea.
Formulation 13: 10 mM AOT (Sodium bis(2-ethylhexyl) sulfosuccinate).
Formulation 14: 0.5-0.1% Tween 20 (nonionic detergent, also known as polysorbate 20 or PEG(20)sorbitan monolauratesorbitan monolaurate).
Formulation 15: 0.5-0.1% Tween 80 (nonionic surfactant, C64H124O26, also known as polyoxyethylene (20) sorbitan monooleate, (x)-sorbitan mono-9-octadecenoate poly(oxy-1,2-ethanediyl), or POE (20) sorbitan monooleate).
Formulation 16: 5-10% Ethanol.
Formulation 17: 20% Glycerin.
Formulation 18: 20% Sorbitol.
Formulation 19: 10% Glycerin/10% Sorbitol.
Formulation 20: 0.1% SLS (Sodium lauryl sulfate).
Formulation 21: 1% Pluronic F127 (nonionic suffactant: α-Hydro-.omega.-hydroxypoly(oxyethylene)poly(oxypropylene)poly(oxyethylene) block copolymer).
Formulation 21: 0.1% Tween 20 (nonionic detergent, also known as Polysorbate 20, or PEG(20)sorbitan monolaurate).
Formulation 21: 10% PG (phospholipid gel).
Mouthrinse neat solution #1 (made in 1× PBS): 7% ETOH, 20% Glycerin, 7% PEG 400, and 1% PLURONIC® F127.
Mouthrinse neat solution #2 (made in 1× PBS): 7% ETOH, 20% Sorbitol, 7% PEG 400, and 1% PLURONIC® F127.
Mouthrinse neat solution #3 (made in 1× PBS): 7% ETOH, 20% Glycerin and 7% PEG 400.
Mouthrinse neat solution #4 (made in 1× PBS): 7% ETOH, 20% Sorbitol and 7% PEG 400.
Other illustrative, but not limiting, mouthrinse formulations are shown in Table 20.
TABLE 20
Illustrative mouthrinse formulations.
Rinse# ETOH Glycerin PEG400 F127 Water1 Fluoride
1 5 22.5 7 1 64.5 187.5
2 6 25 1 0 68 0
3 6 20 7 0 67 0
4 6 20 1 1 72 0
5 7 25 7 0 61 0
6 7 20 1 0 72 0
7 7 20 7 0 66 250
8 5 20 7 1 67 0
9 6.472 21.139 5.361 0.722 66.306 250
10 7 22.5 1 0 69.5 250
11 5 25 1 0 69 250
12 7 20 7 0 66 250
13 5 20 1 1 73 250
14 5 25 7 0.5 62.5 250
15 7 25 1 0.5 66.5 250
16 7 25 7 1 60 250
17 5 25 7 0.5 62.5 0
18 7 20 1 1 71 250
19 6 25 1 1 67 250
20 7 25 7 1 60 125
21 5 25 1 0 69 250
22 5 20 1.5 0.5 73 0
23 7 20 1 1 71 250
24 6 20 1 0 73 250
25 5 22.333 3.778 0.444 68.444 125
26 7 25 1 1 66 0
27 6 25 7 0 62 250
28 7 20 7 1 65 0
29 7 25 4 1 63 62.5
30 5 25 4 0 66 0
31 5 25 1 1 68 0
32 7 25 7 1 60 0
33 7 22.5 4 0.5 66 0
34 5 20 4.5 0 70.5 250
35 5 23 1 0 71 62.5
36 6 20 1 1 72 0
37 5 20 7 1 67 250
38 7 20 1 0 72 0
39 5 25 4 1 65 250
40 5 22.5 7 0 65.5 0
n1 7 20 7 1 65 0
n2 7 20% 7 1 65 0
Sorbitol
n3 7 20 7 0 66 0
n4 7 20% 7 0 66 0
Sorbitol
11xPBS can be substituted for water
In certain embodiments, Corynebacterium-specific STAMPs are formulated in any number of creams, nanoemulsions, lipid micelles, aqueous or no-aqueous gels, sprays, soaps or roll-on bars, or other products used for axilla or other hygiene.
STAMP-mediated selective antimicrobial activity can result in preservation of the normal flora at the oral or axilla mucosal surface, resulting in protective colonization and the conversion of a harmful flora to a beneficial one. Recurrence of pathogen overgrowth would be reduced, which also limits the amount and frequency (and therefore cost) of STAMP delivery. STAMPs allow for “surgical” antimicrobial precision, which limits antimicrobial resistance evolution as well due to the general mechanism of cell membrane damage mediated by the killing region.
A number of anti-S. mutans STAMPs (see Table 21) and anti-C. jeikeium STAMPs have been designed and tested, some in formulations. All show potent selective activity against their bacterial targets in vitro, including against biofilm forms. When tested, STAMPs have little cytotoxicity against cell lines in vitro.
TABLE 21
Illustrative anti-S. mutans STAMPs.
SEQ
STAMP Amino Acid Sequence ID NO
2_1G2 FIKHFIHRFGGGKNLRIIRKGIHIIKKY* 3230
C16AF5 TFFRLFNRSFTQALGKGGGFLKFLKKFFKKLKY* 3231
1845L621 KFINGVLSQFVLERKPYPKLFKFLRKHLL* 3232
1903-21 NIFEYFLEGGGKLFKFLRKHLL* 3233
Single underline is binding peptide.
Double underline is antimicrobial peptide (AMP).
No underline is linker.
*indicates optionally protected (e.g., amidated) C terminal.
TABLE 22
Illustrative anti-C. jeikeium STAMPs.
STAMP Amino Acid Sequence SEQ ID NO
2038L6CAM135 GKAKPYQVRQVLRAVDKLETRRKKGGR 3234
PYPGWRLIKKILRVFKGL*
1619- SKRGRKRKDRRKKKANHGKRPNSGGG 3235
CAM135 GWRLIKKILRVFKGL*
1599-BD2.16 YSKTLHFADGGGKILKFLFKKVF* 3236
1619-BD2.16 SKRGRKRKDRRKKKANHGKRPNSGGG 3237
KILKFLFKKVF*
1904-BD2.16 GSVIKKRRKRMSKKKHRKMLRRTRVQR 3238
RKLGKGGGKILKFLFKKVF*
Single underline is binding peptide.
Double underline is antimicrobial peptide (AMP).
No underline is linker.
*indicates optionally protected (e.g., amidated) C terminal.
It was a surprising discovery that certain anti-S. mutans STAMPs required a salt in the formulation (e.g., PBS) for optimum activity. Thus, for example, the anti-S. mutans STAMP C16G2 (TFFRLFNRSFTQALGKGGGKNLRIIRKGIHIIKKY*, SEQ ID NO:2) comprising the TFFRLFNRSFTQALGK (SEQ ID NO:1) attached to the antimicrobial peptide (AMP) KNLRIIRKGIHIIKKY (SEQ ID NO: 3080) by a peptide linker (GGG) was substantially inactive in water-based salt-free buffers and nanoemulsions, but was active in a phosphate buffered saline (PBS) formulation. Suitable PBS formulations ranged from 0.5× PBS to about 2.5× PBS with an activity optimum at about 1× PBS. Similar results are believed to obtain for other anti-S. mutans STAMPS as well as a number of other STAMPs. In certain embodiments STAMP stability in solution was improved by inclusion of fluoride in mouthrinse.
Example 5 Photodynamic Therapy Targeted Against Streptococcus mutans Dental caries (tooth decay) is one of the most prevalent and costly infectious diseases in the United States. Currently, the annual expenditures on dental services exceed $85 billion, with the majority of these costs attributable to dental caries and its sequelae (www.ada.org/). The oral cavity harbors a complex microbial community consisting of over 600 different non-harmful/commensal microbial species together with a limited number of pathogenic bacteria, including the major etiological agent of dental caries, Streptococcus mutans. Once established, S. mutans generates acid during the fermentation of dietary sugars, which causes the demineralization of tooth structure and inhibits the growth of non-pathogenic commensal bacteria within the same microbial niche. Despite diligent use of broad-spectrum antimicrobial compounds and tooth brushing, S. mutans persists within the oral cavity and causes repeated cycles of cariogenesis. Current “remove all, kill-all” approaches have shown limited efficacy, since a “cleaned” tooth surface provides an equal opportunity for commensal as well as pathogenic bacteria to re-colonize in the non-sterile environment of the oral cavity. To address this shortcoming, we have constructed and evaluated a light-activated S. mutans-selective antimicrobial agent. C16-RB, constructed via conjugation of the S. mutans competence-stimulating peptide to the photodynamic dye rose bengal, displays robust anti-S. mutans activity in vitro under blue exposure from a handheld dental curing light. C16-RB has reduced activity against other oral streptococci under mixed biofilm conditions and has limited cytotoxicity in vitro.
To develop a method of selectively eliminating S. mutans from a dental biofilm so that beneficial species exert a protective colonization effect and long-term protection from S. mutans re-colonization can be attained we created a novel class of targeted antimicrobials, known as specifically-targeted antimicrobial peptides, or STAMPs. STAMPs consist of functionally independent, yet conjoined, domains within a linear peptide sequence; a targeting region and an antimicrobial region. The targeting region, which binds specifically to a bacterial species of interest, delivers the killing portion of the molecule that consists of a normally wide-spectrum antimicrobial peptide. Previously, we successfully designed STAMPs against S. mutans by taking advantage of the competence stimulating pheromone (CSP) peptide produced by this organism that has demonstrated S. mutans-specific recognition. STAMPs synthesized with portions of CSP as targeting domains were capable of specific antimicrobial activity against S. mutans, and not other oral streptococci or non-cariogenic organisms in biofilms.
We hypothesized that targeted killing might be achieved through the use of non-peptide antimicrobial molecules, such as porphyrins or dyes utilized in PDT. Here we present the proof-of-principle construction and in vitro efficacy of the targeted, peptide-guided, photodynamic molecule C16-RB. C16-RB displays S. mutans selective antimicrobial activity upon blue light activation with limited activity against non-cariogenic oral streptococci and epithelial cells.
Materials and Methods Synthesis of C16-RB
All amino acids, synthesis resins and reagents were peptide synthesis grade (Anaspec, San Jose, Calif.; Fisher Scientific). To construct our C16-RB conjugate, conventional 9-fluorenylmethoxy carbonyl (Fmoc) solid-phase methodology was employed to synthesize the CSPC16 peptide and attach the succinate and PEG linkers, utilizing double coupling cycles in N-hdroxybenzotrazole, HBTU (O-benzotriazole-N,N,N,N-tetramethyl-uronium hexafluoro-phosphate) and diisopropyl ethylamine (DIEA), with dimethylformamide (DMF) and N-methylpyrrolidone (NMP) as solvents, as described previously. The peptide resin (1 molar equivalent, 15 mg) was then swollen in DMF for 30 min prior to attachment of the PEG terminal amide group to the carboxyl lactone in RB (FIG. 19B). This reaction was carried out in a mixture of 2-(7-Aza-1H-benzotriazole-1-yl)-1,1,3,3-tetramethyluronium hexafluorophosphate (HATU, 5-molar excess) in dichloromethane (DCM):DMF:dimethylsulphoxide (DMSO) (1:1:1 (v/v)). Ten molar equivalents of DIEA were added to the reaction flask to initiate the reaction, which was protected with argon and stirred at room temperature for 5 h. After completion, the reaction mixture was passed down sintered glass filtered vial and extensively washed with DMF and DCM to remove all waste reagents. The resin was then dried overnight in vacuum, and cleaved with 1 mL of trifluoroacetic acid (TFA)/thioanisole/water/EDT (10/0.5/0.5/025) for 2 hr at room temperature. The cleavage solution was precipitated with 10 mL methyl-tert butyl ether, and the precipitate was washed twice with the same amount of ether. The crude product was purified via preparative-level HPLC (Source 15RPC column, ACTA purifier, Amersham) and eluted with gradient acetonitrile/water from 10 to 35% in 10 min, which was increased to 90% over 8 min before finally being washed 15 min with 95% acetonitrile.
C16-RB was purified further to >90% and the molecular mass confirmed via LC/MS, utilizing increasing hydrophobicity gradient of acetonitrile in water with 0.01% TFA as described above (Waters X-bridge BEH 130 C18 column, 4.6×100mm, particle size 5 μm, Waters 3100 system). LC spectra were analyzed with MassLynx Softward v. 4.1 (Waters). C16-RB mass (3118.0) was confirmed by electrospray ionization (ESI) mass spectroscopy in linear, positive ion mode. The final product was lyophilized and protected from light at all times. C16-RB was soluble in 50% methanol.
Bacterial and Cellular Growth
Streptococcus oralis ATCC 10557, Streptococcus gordonii (Challis), Streptococcus sanguinis (NY101), Streptococcus mitis ATCC 903, Streptococcus salivarius ATCC 13419 and S. mutans wild-type UA140 and JM11 (spectinomycin-resistant) strains were grown in Todd-Hewitt (TH) broth 37° C. in an anaerobic atmosphere of 80% N2, 10% CO2, and 10% H2. BHK-21 (ATCC CRL-10) fibroblasts were propagated in DMEM with 10% FBS, 1 mM sodium pyruvate, 100 units/mL penicillin G, and 100 μg/mL streptomycin at 37° C. with 5% CO2. Cells were detached with 0.25% trypsin and subcultured as recommended by the supplier.
Photodynamic Antimicrobial Assays Against Biofilms
To evaluate C16-RB against monoculture biofilms, S. mutans UA140 was grown overnight in TH prior to inoculation for biofilm formation. For biofilms, 1:5000 dilution of overnight culture was made into TH with 1% sucrose in 2 mL centrifuge tubes (200 μL volume) and grown 24 h under anaerobic conditions. After incubation, biofilms were treated for 5 min with 5 or 25 μM C16-RB or 5 μM RB in 1× PBS, or PBS alone, followed by removal of supernatant and exposure to 5 min blue light (emission 400-550 nm, power 400 mW/cm2) from an Astralis 7 (Ivoclar Vivodent, Austria) handheld LED commonly used as a dental curing light. The light source was suspended 4 cm from the tube bottom (even with the mouth of the tube). A duplicate set of samples were left covered to serve as dark controls. After treatment, biofilms were mechanically disrupted and plated to determine cfu/mL.
To gauge C16-RB selectivity for S. mutans, similar assays were conducted against multispecies biofilms. Mixed biofilms were seeded by diluting (1:5000) a mixture of equal parts S. oralis, S. gordonii, S. mitis, S. sanguinis, S. salivarius, and S. mutans JM11 (made from overnight cultures) into TH with 1% sucrose, 1% glucose, and 1% mannose. Biofilms were incubated and treated as described above with the addition of vitamin C or potassium gluconate. After the addition of agent and 5 min incubation, biofilms were washed 1× with 1× PBS prior to light exposure. After PDT and biofilm disruption, survivors were plated on TH, and TH supplemented with 800 μg/mL spectinomycin, which allowed for quantitation of surviving total oral streptococci and surviving S. mutans, respectively.
Evaluation of C16-RB Cytotoxicity
The effect of RB and C16-RB on human fibroblasts was ascertained by utilizing the Promega CellTiterGlo assay, as described by the manufacturer. Briefly, fibroblasts were grown to confluence, detached, and seeded to ˜5,000 cells per well in a 96-well opaque walled, clear bottom 96-well plate (Nunc International). For long-term dark toxicity, cells were allowed to attach to for 18 h before the culture medium was replaced with medium plus serially-diluted RB or C16-RB (200 μM to 390 nM) or medium alone. After 18-24 h, equal volume Cell Titer Glo reagent was added to each well and mixed. Luciferace activity was then quantified to measure cell viability (Varian Fluorometer in Biolumenescence mode). To measure cytotoxicity after RB or C16-RB light exposure, cells were seeded at ˜10,000 cells per well and allowed to attach for 4 h. Cell growth medium was then replaced with RB or C16-RB containing medium, prior to exposure (a single well at a time) with blue light (400 mW/cm2) suspended ˜3 cm from the well bottom. After exposure, cultures were disrupted with Cell Titer Glo and luciferase activity quantitated as above.
Results Design of Photodynamic Peptide-Dye Conjugate
For the targeting peptide component of the chimeric molecule, we selected a shortened derivative of S. mutans CSP, CSPC16 (sequence: TFFRLFNRSFTQALGK). CSPC16 has been utilized successfully as a STAMP targeting peptide in several constructs, and demonstrates selective binding to S. mutans and not other non-cariogenic bacteria. For the photodynamic dye, we selected rose bengal (RB, FIG. 19A), a xanthene dye with a demonstrated record of safety as a diagnostic tool in optometry. Unlike TBO or methylene blue, RB is not recognized by efflux pumps, and has shown robust activity against a variety of bacteria in vitro in the presence of green or blue light (max absorption ˜549 nm), and can be activated by a handheld dental curing LED.
C16-RB synthesis
As shown in FIG. 19B, RB was attached to the N-terminus of CSPC16 through a succinate/PEG linker to construct the C16-RB molecule. Conventional solid-phase peptide methods were utilized to synthesize CSPC16, followed by linker and RB coupling prior to cleavage from the resin. After cleavage, C16-RB was repeatedly purified by LC/MS prior to evaluation. As shown in FIG. 20, over 95% purity was achieved with the expected mass species observed. The lactone ring in RB was opened as a result of CSPC16 attachment. However, we hypothesized that the conjugate would retain enough singlet-oxygen generating activity for a proof-of-principle demonstration, as other xanthene dyes with activity lack this ring.
C16-RB Efficacy Against Single-Species S. mutans Biofilms
After synthesis, the basic photosensitization potential of C16-RB was assessed by challenging mature single-species S. mutans biofilms (grown 24 h) with C16-RB or unmodified RB, followed by blue emission from a dental curing light. As shown in FIG. 21, potent antimicrobial activity was observed in cultures exposed to C16-RB or RB and blue light: a reduction in over 3 log10 from input cfu/mL at 5 or 25 μM. In contrast, appreciable decreases in cfu/mL were not observed in S. mutans treated with blue light alone, or 5 μM RB or C16-RB dark controls. Modest dark toxicity was observed in samples treated with 25 μM C16-RB. Overall, these results indicate that the peptide-dye conjugate is active against S. mutans and at roughly similar levels to the parental RB molecule.
Selective PDT Against Multi-Species Biofilms
C16-RB was next evaluated for selectivity in mixed cultures containing S. mutans and non-cariogenic oral streptococci that compete for the same niche on the tooth surface. We utilized mixed biofilms of S. mutans transformed with spectinomycin resistance (strain JM11, Merritt, et al., 2005), plus S. oralis, S. gordonii, S. mitis, S. sanguinis, and S. salivarius. The mixed cultures were grown 24 and then treated with RB or C16-RB as indicated, plus potassium gluconate to minimize killing of untargeted bacteria by reducing the superoxide-producing activity of the free C16-RB not bound to S. mutans. Ethanol treatment served as an indiscriminant killing control. As shown in FIG. 21, RB alone exhibited strong indiscriminant photodynamic antimicrobial effects against S. mutans and non-S. mutans in the mixed biofilm system (ratio of surviving S. mutans:non-cariogenic streptococci cfu ˜1). In contrast, C16-RB displayed specific photodynamic activity towards S. mutans, and not the other oral streptococci examined, as reflected in the low ratio of recovered S. mutans to other streptococci. These results suggest C16-RB has antimicrobial activity in the presence of blue light that is specific for S. mutans and dependent on the CSPC16 targeting peptide.
Cytotoxicity Against Eukaryotic Cells
Given the demonstrated PDT potential of RB-C16, experiments were conducted to examine the cytotoxicity for this conjugate and RB alone. IC50s were obtained for BHK cells exposed C16-RB, RB, or Melittin B (positive control for cytotoxicity), with and without blue light exposure. As shown in Table 23, cytotoxicity was noted for cells exposed to Melittin B at the lowest peptide dilution tested at either 5 min or 24 h, with or without light (IC50 <1.56 μM), while light-dependent toxicity was observed only for RB-treated samples. No photo-associated toxicity was noted in BHK cells treated with C16-RB, though modest light-independent cytotoxicity (IC50=90 μM) was detected after 24 h of exposure. These results suggest that C16-RB is not toxic to BHK cells after illumination, and displays mild toxic effects (when compared to Melittin B) after 24 h exposure.
TABLE 23
Cytotoxicity of RB and C16-RB compounds.
IC50 (μM)
BHK
5 min dark:
RB-C16 >100
RB >100
Melittin B <1.56
5 min w/blue light:
RB-C16 >100
RB 40
Melittin B <1.56
24 h dark
RB-C16 55
RB 90
Melittin B <1.56
It is understood that the examples and embodiments described herein are for illustrative purposes only and that various modifications or changes in light thereof will be suggested to persons skilled in the art and are to be included within the spirit and purview of this application and scope of the appended claims. All publications, patents, and patent applications cited herein are hereby incorporated by reference in their entirety for all purposes.
