DISPERSIONS OF RASAGILINE CITRATE

Abstract

The subject invention provides a solid dispersion of rasagiline citrate, a composition and a process for the manufacture thereof.

Description

This application claims benefit of U.S. Provisional Application No. 61/400,369, filed Jul. 27, 2010, the contents of which are hereby incorporated by reference.

Throughout this application various publications, published patent applications, and patents are referenced. The disclosures of these documents in their entireties are hereby incorporated by reference into this application in order to more fully describe the state of the art to which this invention pertains.

BACKGROUND OF THE INVENTION

U.S. Pat. Nos. 5,532,415, 5,387,612, 5,453,446, 5,457,133, 5,599,991, 5,744,500, 5,891,923, 5,668,181, 5,576,353, 5,519,061, 5,786,390, 6,316,504, 6,630,514 disclose R(+)-N-propargyl-1-aminoindan (“R-PAI”), also known as rasagiline. U.S. Pat. No. 6,126,968 and PCT International Application Publication No. WO 95/11016 disclose pharmaceutical compositions comprising rasagiline. Rasagiline has been reported to be a selective inhibitor of the B-form of the enzyme monoamine oxidase (“MAO-B”) and is useful in treating Parkinson's disease and various other conditions by inhibition of MAO-B in the brain.

A formulation of rasagiline mesylate is approved for treating Parkinson's disease either as monotherapy or as an adjunct with other treatments. See, e.g. AZILECT®, Physicians' Desk Reference 2009 (PRD, 63^th Edition).

AZILECT® is indicated for the treatment of the signs and symptoms of idiopathic Parkinson's disease as initial monotherapy and as adjunct therapy to levodopa. Rasagiline, the active ingredient of AZILECT®, is rapidly absorbed, reaching peak plasma concentration (C_max) in approximately 1 hour. The absolute bioavailability of rasagiline is about 36%. (AZILECT® Product Label, May 2006).

While not previously identified as a problem for rasagiline, there remains a need for a solid dispersion of rasagiline with polymeric pharmaceutical excipients that exhibits suitable handling properties.

SUMMARY OF THE INVENTION

The subject invention provides a solid dispersion of at least one polymeric pharmaceutical excipient and rasagiline or a pharmaceutically acceptable salt thereof.

The subject invention also provides a pharmaceutical composition comprising the solid dispersion described herein.

The subject invention further provides a process for making the solid dispersion described herein, comprising:

• • a) dissolving a mixture of rasagiline or the pharmaceutically acceptable salt thereof, and the at least one polymeric pharmaceutical excipient in a solvent to form a solution; and
  • b) removing the solvent from the solution.

The subject invention yet further provides a process for making the solid dispersion described herein, comprising:

• • a) obtaining a solid mixture of rasagiline or the pharmaceutically acceptable salt thereof, and the at least one polymeric pharmaceutical excipient; and
  • b) grinding the mixture.

BRIEF DESCRIPTION OF THE FIGURES

FIG. 1: Cyclic Differential Scanning calorimetry (DSC) thermogram of Rasagiline citrate, sample size 3.43 mg, 20° C./min.

FIG. 2: Modulated Differential Scanning calorimetry (MDSC) thermogram of Rasagiline citrate, sample size 4.00 mg, 2° C./min.

FIG. 3: Trending of glass transition temperature (T_q) by varying polymer content

DETAILED DESCRIPTION OF THE INVENTION

The subject invention provides a solid dispersion of at least one polymeric pharmaceutical excipient and rasagiline or a pharmaceutically acceptable salt thereof.

In an embodiment of the solid dispersion, the at least one polymeric pharmaceutical excipient is a water soluble polymeric pharmaceutical excipient.

In another embodiment of the solid dispersion, the pharmaceutically acceptable salt of rasagiline is rasagiline citrate.

In yet another embodiment of the solid dispersion, the rasagiline citrate is mono-rasagiline citrate.

In yet another embodiment of the solid dispersion, the at least one polymeric pharmaceutical excipient is polyvinylpyrrolidone, hydroxypropyl methylcellulose, hydroxypropyl methylcellulose acetate succinate, or hydroxypropyl methylcellulose phthalate.

In yet another embodiment of the solid dispersion, the at least one polymeric pharmaceutical excipient is a co-polymer.

In yet another embodiment of the solid dispersion, the co-polymer is polyvinylpyrrolidone-vinyl acetate or methacrylic acid-ethyl acrylate.

In yet another embodiment of the solid dispersion, the co-polymer is methacrylic acid-ethyl acrylate.

In yet another embodiment of the solid dispersion, T_g of the solid dispersion is at least 20° C. higher than that of rasagiline or a pharmaceutically acceptable salt thereof.

The subject invention also provides a pharmaceutical composition comprising the solid dispersion described herein.

The subject invention further provides a process for making the solid dispersion of rasagiline citrate described herein, comprising:

• • a) combining a mixture of rasagiline free base and the at least one polymeric pharmaceutical excipient in a solvent to form a solution;
  • b) adding citric acid to the solution; and
  • c) removing the solvent from the solution.

The subject invention further provides a process for making the solid dispersion of rasagiline citrate described herein, comprising:

• • a) dissolving a mixture of rasagiline or the pharmaceutically acceptable salt thereof, and the at least one polymeric pharmaceutical excipient in a solvent to form a solution; and
  • b) removing the solvent from the solution.

In an embodiment of the process, the pharmaceutically acceptable salt of rasagiline is rasagiline citrate.

In another embodiment of the process, the rasagiline citrate is mono-rasagiline citrate.

In an embodiment of the process, the solvent is methanol, ethanol, acetone, dichloromethane, dioxane and water, or a mixture of at least two thereof.

In another embodiment of the process, step b) is performed at a temperature of between about 55° C. and 80° C. by rotary evaporation.

In yet another embodiment of the process, in step b) the solvent is removed by lyophilization.

The subject invention yet further provides a process for making the solid dispersion of rasagiline citrate described herein, comprising:

• • a) combining a mixture of rasagiline free base, the at least one polymeric pharmaceutical excipient, and citric acid; and
  • b) grinding the mixture.

The subject invention yet further provides a process for making the solid dispersion of rasagiline citrate described herein, comprising:

• • a) obtaining a solid mixture of rasagiline or the pharmaceutically acceptable salt thereof, and the at least one polymeric pharmaceutical excipient; and
  • b) grinding the mixture.

In an embodiment of the process, the pharmaceutically acceptable salt of rasagiline is rasagiline citrate.

In another embodiment of the process, the rasagiline citrate is mono-rasagiline citrate.

In yet another embodiment of the process, step b) is performed by dry milling the mixture.

In yet another embodiment of the process, step b) is performed by wet milling the mixture with a solvent.

In yet another embodiment of the process, the solvent is methanol or acetone.

In yet another embodiment of the process, step b) is performed at a temperature below 0° C.

In yet another embodiment of the process, step b) is performed at a temperature below −10° C.

In yet another embodiment of the process, step b) is performed at a temperature below −25° C.

In yet another embodiment of the process, step b) is performed at a temperature below −50° C.

In yet another embodiment of the process, step b) is performed at a temperature below −100° C.

In yet another embodiment of the process, step b) is performed at a temperature below −150° C.

The subject invention yet further provides a method of treating a human subject afflicted with Parkinson's disease comprising administering to the human subject an amount of the pharmaceutical composition of claim 8, effective to treat the human subject.

By any range disclosed herein, it is meant that all hundredth, tenth and integer unit amounts within the range are specifically disclosed as part of the invention. Thus, for example, 0.01 mg to 50 mg means that 0.02, 0.03 . . . 0.09; 0.1, 0.2 . . . 0.9; and 1, 2 . . . 49 mg unit amounts are included as embodiments of this invention.

Citric acid is a weak organic acid, and is triprotic. Therefore, the rasagiline citrate described herein may exist in mono-, di- or tri-rasagiline citrate form or a mixture thereof.

As used herein, an example of an immediate release formulation of rasagiline is an AZILECT® Tablet containing rasagiline mesylate.

As used herein, a polymer is a large molecule composed of repeating structural units typically connected by covalent chemical bonds.

As used herein, a “pharmaceutically acceptable” carrier or excipient is one that is suitable for use with humans and/or animals without undue adverse side effects (such as toxicity, irritation, and allergic response) commensurate with a reasonable benefit/risk ratio.

As used herein, a “pharmaceutically acceptable salt” of rasagiline includes citrate, tannate, malate, mesylate, maleate, fumarate, tartrate, esylate, p-toluenesulfonate, benzoate, acetate, phosphate and sulfate salts. For the preparation of pharmaceutically acceptable acid addition salts of the compounds of the invention, the free base can be reacted with the desired acids in the presence of a suitable solvent by conventional methods.

Rasagiline can also be used in its free base form. A process of manufacture of the rasagiline free base is described in POT publication WO 2008/076348, the contents of which are hereby incorporated by reference.

As used herein, an “isolated” compound is a compound that has been separated from the crude reaction mixture in which it formed by an affirmative act of isolation. The act of isolation necessarily involves separating the compound from the other known components of the crude reaction mixture, with some impurities, unknown side products and residual amounts of the other known components of the crude reaction mixture permitted to remain. Purification is an example of an affirmative act of isolation.

As used herein, a composition that is “free” of a chemical entity means that the composition contains, if at all, an amount of the chemical entity which cannot be avoided following an affirmative act intended to separate the chemical entity and the composition.

As used herein, a “glass transition temperature (T_g)” of a solid is the temperature where the solid goes from a rigid state to a flexible state. At T_g, a polymer undergoes a phase transition from a hard, glass-like state to a flexible, rubber-like state. The T_g temperature values listed herein were determined based upon half-height of the step change or “S” shape curve seen in DSC data.

As used herein, a polymer is a large molecule composed of repeating structural units typically connected by covalent chemical bonds.

As used herein, a “solid dispersion” is a drug-containing pharmaceutical bulk substance in which the drug is dispersed in a pharmaceutical excipient such as a polymer, a co-polymer, or a mixture thereof.

Specific examples of pharmaceutically acceptable carriers and excipients that may be used to formulate oral dosage forms of the present invention are described, e.g., in U.S. Pat. No. 6,126,968 to Peskin et al., issued Oct. 3, 2000. Techniques and compositions for making dosage forms useful in the present invention are described, for example, in the following references: 7 Modern Pharmaceutics, Chapters 9 and 10 (Banker & Rhodes, Editors, 1979); Pharmaceutical Dosage Forms: Tablets (Lieberman et al., 1981); Ansel, Introduction to Pharmaceutical Dosage Forms 2nd Edition (1976); Remington's Pharmaceutical Sciences, 17th ed. (Mack Publishing Company, Easton, Pa., 1985); Advances in Pharmaceutical Sciences (David Ganderton, Trevor Jones, Eds., 1992); Advances in Pharmaceutical Sciences Vol 7. (David Ganderton, Trevor Jones, James McGinity, Eds., 1995); Aqueous Polymeric Coatings for Pharmaceutical Dosage Forms (Drugs and the Pharmaceutical Sciences, Series 36 (James McGinity, Ed., 1989); Pharmaceutical Particulate Carriers: Therapeutic Applications: Drugs and the Pharmaceutical Sciences, Vol 61 (Alain Rolland, Ed., 1993); Drug Delivery to the Gastrointestinal Tract (Ellis Horwood Books in the Biological Sciences. Series in Pharmaceutical Technology; J. G. Hardy, S. S. Davis, Clive G. Wilson, Eds.); Modern Pharmaceutics Drugs and the Pharmaceutical Sciences, Vol 40 (Gilbert S. Banker, Christopher T. Rhodes, Eds.).

The pharmaceutical dosage forms may be prepared as medicaments to be administered orally, parenterally, rectally or transdermally. Suitable forms for oral administration include tablets, compressed or coated pills, dragees, sachets, hard or soft gelatin capsules, sublingual tablets, syrups and suspensions; for parenteral administration the invention provides ampoules or vials that include an aqueous or non-aqueous solution or emulsion; for rectal administration the invention provides suppositories with hydrophilic or hydrophobic vehicles; for topical application as ointments; and for transdermal delivery the invention provides suitable delivery systems as known in the art.

Tablets may contain suitable binders, lubricants, disintegrating agents, coloring agents, flavoring agents, flow-inducing agents, melting agents, stabilizing agents, solubilizing agents, antioxidants, buffering agent, chelating agents, fillers and plasticizers. For instance, for oral administration in the dosage unit form of a tablet or capsule, the active drug component can be combined with an oral, non-toxic, pharmaceutically acceptable, inert carrier such as gelatin, agar, starch, methyl cellulose, dicalcium phosphate, calcium sulfate, mannitol, sorbitol, microcrystalline cellulose and the like. Suitable binders include starch, gelatin, natural sugars such as corn starch, natural and synthetic gums such as acacia, tragacanth, or sodium alginate, povidone, carboxymethylcellulose, polyethylene glycol, waxes, and the like. Antioxidants include ascorbic acid, fumaric acid, citric acid, malic acid, gallic acid and its salts and esters, butylated hydroxyanisole, editic acid. Lubricants used in these dosage forms include sodium oleate, sodium stearate, sodium benzoate, sodium acetate, stearic acid, sodium stearyl fumarate, talc and the like. Disintegrators include, without limitation, starch, methyl cellulose, agar, bentonite, xanthan gum, croscarmellose sodium, sodium starch glycolate and the like, suitable plasticizers include triacetin, triethyl citrate, dibutyl sebacate, polyethylene glycol and the like.

One type of oral dosage forms of the present invention relates to delayed release formulations. Such formulations may be comprised of an acid resistant excipient which prevents the dosage form or parts thereof from contacting the acidic environment of the stomach. The acid resistant excipient may coat the rasagiline in the form of an enteric coated tablet, capsule, or gelatin capsule. Enteric coating, in the context of this invention, is a coating which prevents the dissolution of an active ingredient in the stomach. Specific examples of pharmaceutically acceptable carriers and excipients that may be used to formulate such delayed release formulations are described, e.g., in International Application Publication No. WO 06/014973, hereby incorporated by reference in its entirety.

Another type of oral dosage forms of the present invention relates to fast disintegrating formulations which provide a means to avoid the absorption of rasagiline in the stomach, and to eliminate the need for swallowing tablets, by absorption of rasagiline into the body before reaching the stomach. Such absorption of rasagiline can be accomplished by contact with the buccal, sublingual, pharyngeal and/or esophageal mucous membranes. To accomplish this, the fast disintegrating formulations were designed to rapidly disperse within the mouth to allow maximum contact of rasagiline with the buccal, sublingual, pharyngeal and/or esophageal mucous membranes. Specific examples of pharmaceutically acceptable carriers and excipients that may be used to formulate such fast disintegrating formulations are described, e.g., in International Application Publication No. WO 03/051338, hereby incorporated by reference in its entirety.

Other pharmaceutical compositions of the present invention include transdermal patches. Transdermal patches are medicated adhesive patches placed on the skin to deliver a time-released dose of medication through the skin and into the bloodstream. A wide variety of pharmaceuticals can be delivered through transdermal patches. Some pharmaceuticals must be combined with other substances, for example alcohol, to increase their ability to penetrate the skin. Transdermal patches have several important components, including a liner to protect the patch during storage, the drug, adhesive, a membrane (to control release of the drug from the reservoir), and a backing to protect the patch from the outer environment. The two most common types of transdermal patches are matrix and reservoir types. (Wikipedia; and Remington, The Science and Practice Pharmacy, 20^th Edition, 2000)

In reservoir type patches, a drug is combined with a non-volatile, inert liquid, such as mineral oil, whereas in matrix type patches a drug is dispersed in a lipophilic or hydrophilic polymer matrix such as acrylic or vinylic polymers. Adhesive polymers, such as polyisobutylene, are used to hold the patch in place on the skin. (Stanley Scheindlin, (2004) “Transdermal Drug Delivery: PAST, PRESENT, FUTURE,” Molecular Interventions, 4:308-312)

The major limitation to transdermal drug-delivery is the intrinsic barrier property of the skin. Penetration enhancers are often added to transdermal drug formulations in order to disrupt the skin surface and cause faster drug delivery. Typical penetration enhancers include high-boiling alcohols, diols, fatty acid esters, oleic acid and glyceride-based solvents, and are commonly added at a concentration of one to 20 percent (w/w). (Melinda Hopp, “Developing Custom Adhesive Systems for Transdermal Drug Delivery Products,” Drug Delivery)

In all of its aspects, the present invention provides pharmaceutical dosage forms useful for treating a condition selected from the group consisting of: Parkinson's disease (PD), brain ischemia, stroke, head trauma injury, spinal trauma injury, neurotrauma, neurodegenerative disease, neurotoxic injury, nerve damage, dementia, Alzheimer's type dementia, senile dementia, depression, memory disorders, hyperactive syndrome, attention deficit disorder, Multiple Sclerosis (MS), schizophrenia, affective illness, Amyotrophic Lateral Sclerosis, Restless Legs Syndrome (RLS), hearing loss, Multiple System Atrophy (MSA), Glucoma, modifying Parkinson's disease, and Progressive Supranuclear Palsy (PEP), but with a reduced risk of peripheral MAO inhibition that is typically associated with administration of rasagiline with known oral dosage forms.

A conventional method for the manufacture of a solid dispersion relates to a fusion process which is characterized by melting a drug substance and a polymeric pharmaceutical excipient together at elevated temperature and, then, cooling the melt to solidify. Another conventional method for the manufacture of a solid dispersion relates to a solvent process which is characterized by dissolving a drug substance and a polymeric pharmaceutical excipient in an appropriate solvent and, then, removing the solvent. Additional method for the manufacture of a solid dispersion relates to mixing a drug substance and a polymeric pharmaceutical excipient through milling.

Generally, a phase-separated dispersion will exhibit two T_g values, whereas a molecular dispersion will exhibit a single T_g.

The subject invention is also intended to include all isotopes of atoms occurring on the compounds disclosed herein. Isotopes include those atoms having the same atomic number but different mass numbers. By way of general example and without limitation, isotopes of hydrogen include tritium and deuterium. Isotopes of carbon include C-13 and C-14.

It will be noted that any notation of a carbon in structures throughout this application, when used without further notation, are intended to represent all isotopes of carbon, such as ¹²C, ¹³C, or ¹⁴C. Furthermore, any compounds containing ¹³C or ¹⁴C may specifically have the structure of any of the compounds disclosed herein.

It will also be noted that any notation of a hydrogen in structures throughout this application, when used without further notation, are intended to represent all isotopes of hydrogen, such as ¹H, ²H, or ³H. Furthermore, any compounds containing ²H or ³H may specifically have the structure of any of the compounds disclosed herein.

Isotopically-labeled compounds can generally be prepared by conventional techniques known to those skilled in the art or by processes analogous to those described in the Examples disclosed herein using an appropriate isotopically-labeled reagents in place of the non-labeled reagents employed.

This invention will be better understood from the experimental details which follow. However, one skilled in the art will readily appreciate that the specific methods and results discussed are merely illustrative of the invention as described more fully in the claims which follow thereafter.

Experimental Details

A solid dispersion screen was carried out using rasagiline citrate and pharmaceutical excipients of polymers. Dispersions were prepared using several techniques including rotary evaporation from solution, cryogrinding dry components and lyophilization. Samples were analyzed by modulated Differential Scanning calorimetry (DSC) to determine glass transition temperatures (T_g). A slight excess of citric acid was used in most dispersions i.e. 0.7:1 mol of rasagiline: citric acid.

The pharmaceutical excipients of polymers used in the following example are listed in the table below:

Excipient             Abbreviation
polyvinylpyrrolidone- PVP-VA
vinyl acetate
polyvinylpyrrolidone  PVP K-29/32
polyvinylpyrrolidone  PVP K-90
hydroxypropyl         HPMC
methylcellulose
hydroxypropyl         HPMC-AS
methylcellulose-
acetate succinate
hydroxypropyl         HPMC-P
methylcellulose-
phthalate
methacrylic acid      Eudragit
ethyl acrylate        L-100
copolymer

These pharmaceutical excipients of polymers each exhibits characteristics as listed in the following table.

Excipient      Observationa
Eudragit L-100 small white particles, no
               B/E
HPMC           small rod-like fragments,
               B/E
HPMC-AS        small particles, some B/E
HPMC-P         small, irregular
               fragments, B/E
PVP K-29/32    small particles, B/E
PVP K-90       small particles, B/E
aObservations by light microscopy. B = birefringence, E = extinction.

Example 1

Preparation of Mono-Rasagiline Citrate Salt

In the following experiment, rasagiline base was mixed with citric acid (1:1 mol:mol) and then methanol was added to the mixture. After stirring and complete dissolution of solids, the solution was evaporated under vacuum in rotary evaporator at bath temperature 60° C. The resulting foamy substance was dried under vacuum to obtain mono-rasagiline citrate.

TABLE 1
Preparation of Mono-Rasagiline Citrate Salt
Sample	Solvent/
No	Conditionsa	Observations	Analysisb	Result
1	MeOH/RE	foamy	HSM	At 40° C.,
	@60° C.,	substance		solids
	vacuum			become gel-
	dried			like, all
				become gel
				at 80° C.
			cyclic	Tg = 18° C.
			DSC
			Modulated	Tg = 16° C.
			DSC
aRE = rotary evaporation,
bHSM = hotstage microscopy, DSC = differential scanning calorimetry.

Example 2

Solid Dispersion of Rasagiline Citrate Prepared by Rotary Evaporation

The experiments conducted in this example are listed below in Table 2. In each of the experiments, rasagiline free base, excipient, and citric acid were combined and mixed in the corresponding solvent. A solid dispersion was prepared from the mixture by rotary evaporation of the solvent at conditions listed in Table 2 below.

TABLE 2
	Exp.
Excipienta	No.*	Solventb	Conditionsd	Observatione
Eudragit	1	EtOH	RE @70° C.	glassy solids, some which show
L-100				extinction
(1:1)			vac. dried	glassy solids
Eudragit	2c	MeOH	RE @65° C.,	handleable white powder, glassy
L-100			vac. dried	fragments, a few extinguish
(70:30)
Eudragit	3c	MeOH	RE @60° C.,	white solid, stored @ −13° C.
L-100			vac. dried
(75:25)
HPMC	4	MeOH:H2O	did not	—
(1:1)			dissolve,
			sample
			discarded
HPMC	5	MeOH:DCM	RE @60° C.,	gel formed, plastic-like film
(75:25)			vac. dried	after vac dried w/B, stored @ −13° C.
HPMC	6	MeOH:H2O	sample did	—
(70:30)			not dissolve
HPMC-AS	7	MeOH:ACN	RE @80° C.	foamy subtance, very sticky
(1:1)			vac. dried	gel
HPMC-AS	8c	Acetone:MeOH	RE @55° C.,	many solids clung to side of
(70:30)			vac. dried	vial, scraped down solids are
				handleable and off-white.
				Glassy fragments, no B/E
HPMC-AS	9c	MeOH:DCM	RE @60° C.,	white foam, dry white powder
(75:25)			vac. dried	when dried
HPMC-P	10	Acetone:H2O	RE @50° C.	foam with solid particles
(1:1)				dispersed, became gel
HPMC-P	11	MeOH:DCM	RE @60° C.,	white foam, white powder when
(75:25)			vac. dried	dried
HPMC-P	12c	Acetone:DCM	RE @55° C.,	tacky white solids, glassy
(90:10)			vac. dried	fragments
PVP-VA	13	EtOH	RE @70° C.	glassy solids, slightly sticky
(1:1)				to spatula, no B/E under
				microscope
			vac. dride	glassy solids
	14c	DCM	—	sample did not dissolve
PVP-VA	15c	Acetone:MeOH	RE @55° C.,	handleable white solids, glassy
(70:30)			vac. dried	fragments, no B/E
PVP-VA	16c	Acetone:DCM	RE @55° C.,	fine white powder, easily
(90:10)			vac. dried	handled, unifom glassy
				fragments
PVP	17	Acetone:EtOH	RE @60° C.	foamy substance, gel like
K-29/32			vac. dried	glassy material, became powder
(1:1)				when touched with spatula.
				Glassy solids under microscope,
				no B/E
PVP	18	Acetone:MeOH	RE @60° C., vac	white sticky solid, no B/E, dry
K-29/32			dried	white solid when dried, stored @
(75:25)				−13° C.
PVP K-90	19	Acetone:EtOH	RE @70° C.	glassy solids, no B/E
(1:1)
PVP K-90	20c	DCM:MeOH	RE @50° C.,	handleable white powder, glassy
(70:30)			vac. dried	fragments, few extinguish
PVP K-90	21c	MeOH:acetone	RE @60° C.,	white foam, no B/E, dy white
(75:25)			vac. dried	solid when dried, stored @ −13° C.
PVP K-90	22c	Acetone:DCM	RE @55° C.,	tacky white solids, glassy
(90:10)			vac. dried	fragments
*the molar ratio of rasagiline:citric acid is 1:1 unless indicated otherwise
aExcipient: Rasagiline ratio (weight/weight)
bExcipient and Rasagiline dissolved in solvent, followed by addition of citric acid in a 1:1 molar ratio.
c0.7:1 molar ratio of rasagiline:citric acid
dRE = rotary evaporation.
eobservations by light microscopy. B = birefringence, E = extinction

Example 3

Solid Dispersion of Rasagiline Citrate Prepared by Grinding

The experiments conducted in this example are listed below in Table 3, In each of the experiments, rasagiline free base, excipient, and citric acid were combined and mixed. A solid dispersion was prepared from the mixture by dry milling, wet milling, or cryo-grinding the mixture at conditions listed in Table 3 below.

TABLE 3
	Exp.
Excipienta	No.*	Conditions	Observationc
HPMC	1b	dry milled, 30 Hz,	white powder, solids present
(60:40)		15 minutes	with, B/E, no single phase
	2	wet milled w/	fine white powder and sticky
		acetone, 30 Hz, 10	solids, fragments with B/E
		minutes	present
HPMC	3	cryogrind grind 2	small white particles, no B/E
(70:30)		minutes, 5 cycles,
		rate = 10
HPMC-P	4	cryogrind grind 2	small white particles, no B/E
(1:1)		minutes, 3 cycles,
		rate = 10
HPMC-P	5	cryogrind grind 2	small white particles, approx
(70:30)		minutes, 5 cycles,	same size, shape, no B/E
		rate = 10
PVP-VA	6b	dry milled, 30 Hz,	white powder, solids present
(1:1)		15 minutes	with B/E, pockets of differing
			morphology
	7	wet milled w/ MeOH,	fine white powder and sticky
		30 Hz, 10 minutes	solids, pockets of
			birefringent material
PVP-VA	8	cryogrind grind 2	white fine particles with no
(70:30)		minutes, 5 cycles,	B/E
		rate = 10
PVP	9	cryogrind grind 2	small white particles approx
K-29/32		minutes, 5 cycles,	same size, no B/E
(70:30)		rate = 10
PVP K-90	10b	cryogrind grind 2	white fine powder. Appears as
(60:40)		minutes, 5 cycles,	single phase with same size,
		rate = 10	morphology
*the molar ratio of rasagiline:citric acid is 1:1 unless indicated otherwise
aExcipient: Rasagiline ratio (weight/weight)
b0.7:1 molar ratio of Rasagiline:citric acid
cobservations by light microscopy. B = birefringence, E = extinction

Example 4

Solid Dispersion of Rasagiline Citrate Prepared by Lyophilization

The experiments conducted in this example are listed below in Table 4. In each of the experiments, rasagiline free base, excipient, and citric acid were combined and mixed in the corresponding solvent. A solid dispersion was prepared from the mixture by lyophilization at conditions listed in Table 4 below.

TABLE 4
Excipienta	Exp. No.	Solvent	Conditions	Observation
HPMC-P	1b	dioxane	lyophilize	fluffy white powder
(7:3)			overnight
HPMC-AS	2b	dioxane	lyophilize	fluffy white powder
(7:3)			overnight
HPMC-P	3b	dioxane-	lyophilize	fluffy white powder
(7:3)		water	overnight
		(1:1)
PVP-VA	4b	dioxane-	lyophilize	fluffy white powder
(7:3)		water	overnight
		(1:1)
aExcipient: Rasagiline ratio (weight/weight)
b0.7:1 molar ratio of Rasagiline:citric acid

Example 5

Analysis of Dispersions of Rasagiline Citrate

Samples of dispersion of rasagiline citrate obtained in Examples 2-4 were analyzed and the results are summarized in Table 5 below.

TABLE 5
Excipienta	Sample No.	Prep Methodb	Analysis	Result	Tg calcc
Eudragit ® L	1d	RE	MDSC	Tg = 15° C.	60° C.
100
(1:1)
Eudragit ® L	2	RE	MDSC	Tg = 19° C.	82° C.
100
(30:70)
HPMC	3	cryomill	MDSC	Tg = 32° C.,	106° C.
(30:70)				126° C.
HPMC-AS	4	RE	MDSC	Tg = 17° C.	90° C.
(30:70)				100° C.
HPMC-AS	5	lyophilization	MDSC	Tg = 17° C.	90° C.
(30:70)
HPMC-P	6d	cryomill	MDSC	Tg = 25° C.	69° C.
(1:1)
HPMC-P	7	RE	MDSC	Tg = 8° C.	103° C.
(25:75)
HPMC-P	8	lyophilization	MDSC	Tg = 29° C.	96° C.
(30:70)
HPMC-P	9	cryomill	MDSC	Tg = 27° C.	96° C.
(30:70)
HPMC-P	10d	RE	MDSC	—	127° C.
(10:90)
PVP K-29/32	11d	RE	MDSC	Tg = 3° C.	75° C.
(1:1)
PVP K-29/32	12	cryomill	MDSC	Tg = 29° C.	106° C.
(30:70)
PVP K-29/32	13	lyophilization	MDSC	Tg = 30° C.	106° C.
(30:70)
PVP K-29/32	14	RE	MDSC	Tg = 17° C.	106° C.
(25:75)
PVP K-90	15d	RE	MDSC	Tg = 18° C.	78° C.
(1:1)
PVP K-90	16	RE	MDSC	Tg = 34° C.	111° C.
(30:70)
PVP K-90	17	cryomill	MDSC	Tg = 39° C.	94° C.
(40:60)
PVP K-90	18	RE	MDSC	—	151° C.
(10:90)
PVP-VA	19d	RE	MDSC	Tg = 16° C.,	56° C.
(1:1)				77° C.
PVP-VA	20	RE	MDSC	Tg = 38° C.,	76° C.
(30:70)
PVP-VA	21	lyophilization	MDSC	Tg = 22° C.,	76° C.
(30:70)
PVP-VA	22	cryomill	MDSC	Tg = 26° C.,	76° C.
(30:70)
aRasagiline: excipient weight ratio listed in parentheses.
bRE = rotary evaporation.
cTg value for ideal dispersion calculated using Fox equation.
d1:1 molar ratio of Rasagiline:citric acid. All other samples contain slight excess of citric acid

Example 6

Stressing of Dispersions of Rasagiline Citrate

Stability of the dispersions of rasagiline citrate obtained in Examples 2-4 was studied at the conditions listed in Table 6 below. The results are also summarized in Table 6 below.

TABLE 6
	Sample
Excipienta	No.	Conditionsb	Duration	Observationc
Eudragit	1	75% RH	2	hours	no change
L-100			4	hours	no change
(70:30)			6	hours	no change
			8	hours	no change
			24	hours	pooling of solids,
					needles present
			5	days	slight pooling of
					solids w/ moisture
HPMC-AS	2	75% RH	2	hours	no change
(70:30)			4	hours	no change
			6	hours	no change
			8	hours	no change
			24	hours	pooling of solids w/
					moisture
			5	days	pooling of solids w/
					moisture
HPMC-P	3	75% RH	2	hours	no change
(70:30)			4	hours	no change
			6	hours	no change
			8	hours	pooling of solids
			24	hours	pooling of solids w/
					moisture
			5	days	deliquesced
PVP K-29/32	4	75% RH	2	hours	no change
(70:30)			4	hours	pooling of solids
			6	hours	pooling of solids
			8	hours	pooling of solids
			24	hours	deliquesced
PVP K-90	5	75% RH	2	hours	no change
(70:30)			4	hours	no change
			6	hours	no change
			8	hours	no change
			24	hours	deliquesced
PVP-VA	6	75% RH	2	hours	no change
(70:30)			4	hours	no change
			6	hours	pooling of solids
			8	hours	pooling of solids
			24	hours	deliquesced
Rasagiline	7	75% RH	2	hours	pooling of solids
Citrate			4	hours	deliquesced
			6	hours	deliquesced
			8	hours	deliquesced
			24	hours	deliquesced
HPMC-P	8	75% RH	1	day	solids pooling
(1:1)					together with
					moisture
PVP-VA	9	75% RH	1	day	solids deliquesced
(70:30)
PVP K-90	10	75% RH	1	day	slight pooling of
(70:30)					moisture around
					solids
apolymer: drug weight ratio listed in parentheses.
bRH = relative humidity.
cObservations made visually using light microscopy.

Example 7

Additional Preparation of Solid Dispersion of Rasagiline Citrate

In Examples 2-4, rasagiline citrate was formed in-situ by combining rasagiline free base, excipient, and citric acid in the preparation of solid dispersion of rasagiline citrate. Alternatively, the solid dispersion of rasagiline citrate can be prepared by obtaining rasagiline citrate salt first. The rasagiline citrate can be obtained by reacting rasagiline free base with citric acid in the presence of a suitable solvent by conventional methods, e.g. the process described in Example 1.

The rasagiline citrate obtained can then be mixed with the excipient listed in Table 2 to prepare the solid dispersion of rasagiline citrate by the rotary evaporation as described in Example 2. The rasagiline citrate obtained can also be mixed with the excipient listed in Table 3 to prepare the solid dispersion of rasagiline citrate by dry milling, wet milling, or cryo-grinding as described in Example 3. The rasagiline citrate obtained can further be mixed with the excipient listed in Table 4 to prepare the solid dispersion of rasagiline citrate by lyophilization as described in Example 4.

Discussion of Examples 1-6

The plasticizing effect of water as well as the low T_g of rasagiline citrate has generally resulted in dispersions with low T_g values. T_g of mono-rasagiline citrate was ˜17° C. by DSC.

Most of the solid dispersions of rasagiline citrate prepared appeared to be phase-separated by MDSC. In addition, T_g of some of the solid dispersions of rasagiline citrate prepared was not observed due to decomposition of rasagiline at elevated temperatures.

Dispersions containing PVP K90 and PVP-VA have shown the largest increase in T_g with high polymer loadings but both deliquesced when stressed under high relative humidity for 1 day.

All solid dispersions of rasagiline citrate prepared using methods described in Examples 2-4 have resulted in handleable white powders.

As T_g can be impacted by technique used to generate dispersions, dispersions were prepared by different methods. For most polymers, little difference in T_g was noted with different methods of preparation. However, for HPMC-P an increase in T_g of ˜20° C. was observed for a lyophilized sample compared with a sample prepared by rotary evaporation.

Preparation of solid dispersions involving HPMC was difficult due to the low solubility of HPMC in most solvents. A dispersion was prepared by cryogrinding but it did not exhibit a T_u much higher than that of the rasagiline base.

Solid dispersions of rasagiline citrate prepared were stressed at 75% relative humidity over a period of 24 hours and were compared with rasagiline citrate alone. All solid dispersions except for PVP K-29/32 and PVP-VA showed no moisture accumulation for the first 6 hours by visual inspection. After 6 hours, pooling of moisture was observed in some samples and deliquescence was observed in some samples after 24 hours.

Dispersions containing Eudragit L-100 and HPMC-AS showed no change after 24 hours. All dispersions showed greater stability than rasagiline citrate alone, which was fully deliquesced after 4 hours.

T₄ of varying polymer loadings was also studied. As shown in FIG. 3, three dispersions showed a significant increase of T_g with increasing loading of polymers: dispersions containing PVP K-29/32, PVP-VA, and PVP-K90.

Stability of dispersions under high relative humility was also studied. The results showed that dispersions containing Eudragit L-100 were the most stable and dispersions containing PVP K-29/32 were the least stable. The relative ranking of stability is as follows: Eudragit L-100>HPMC-AS>PVP K-90>HPMCP>PVP-VA>PVP K-29/32.

Claims

1. A solid dispersion of at least one polymeric pharmaceutical excipient and rasagiline or a pharmaceutically acceptable salt thereof.

2. The solid dispersion of claim 1, wherein the at least one polymeric pharmaceutical excipient is a water soluble polymeric pharmaceutical excipient.

3. The solid dispersion of claim 1 or 2, wherein the pharmaceutically acceptable salt of rasagiline is rasagiline citrate.

4. The solid dispersion of claim 3, wherein the rasagiline citrate is mono-rasagiline citrate.

5. The solid dispersion of any one of claims 1-4, wherein the at least one polymeric pharmaceutical excipient is polyvinylpyrrolidone, hydroxypropyl methylcellulose, hydroxypropyl methylcellulose acetate succinate, or hydroxypropyl methylcellulose phthalate.

6. The solid dispersion of any one of claims 1-4, wherein the at least one polymeric pharmaceutical excipient is a co-polymer.

7. The solid dispersion of claim 6, wherein the co-polymer is polyvinylpyrrolidone-vinyl acetate or methacrylic acid-ethyl acrylate.

8. The solid dispersion of claim 7, wherein the co-polymer is methacrylic acid-ethyl acrylate.

9. The solid dispersion of any one of claims 1-8, wherein Tg of the solid dispersion is at least 20° C. higher than that of rasagiline or a pharmaceutically acceptable salt thereof.

10. A pharmaceutical composition comprising the solid dispersion of any one of claims 1-9.

11. A process for making the solid dispersion of any one of claims 1-9, comprising:

a) combining a mixture of rasagiline free base and the at least one polymeric pharmaceutical excipient in a solvent to form a solution;

b) adding citric acid to the solution; and

c) removing the solvent from the solution.

12. The process of claim 11, wherein the solvent is methanol, ethanol, acetone, dichloromethane, dioxane and water, or a mixture of at least two thereof.

13. The process of claim 11 or 13, wherein step c) is performed at a temperature of between about 55° C. and 80° C. by rotary evaporation.

14. The process of claim 11 or 12, wherein in step b) the solvent is removed by lyophilization.

15. A process for making the solid dispersion of any one of claims 1-9, comprising:

a) dissolving a mixture of rasagiline or the pharmaceutically acceptable salt thereof, and the at least one polymeric pharmaceutical excipient in a solvent to form a solution; and

b) removing the solvent from the solution.

16. The process of claim 15, wherein the pharmaceutically acceptable salt of rasagiline is rasagiline citrate.

17. The process of claim 16, wherein the rasagiline citrate is mono-rasagiline citrate.

18. The process of any one of claims 15-17, wherein the solvent is methanol, ethanol, acetone, dichloromethane, dioxane and water, or a mixture of at least two thereof.

19. The process of any one of claims 15-18, wherein step b) is performed at a temperature of between about 55° C. and 80° C. by rotary evaporation.

20. The process of any one of claims 15-18, wherein in step b) the solvent is removed by lyophilization.

21. A process for making the solid dispersion of any one claims 1-9, comprising:

a) combining a mixture of rasagiline free base, the at least one polymeric pharmaceutical excipient, and citric acid; and

b) grinding the mixture.

22. The process of claim 21, wherein step b) is performed by dry milling the mixture.

23. The process of claim 21, wherein step b) is performed by wet milling the mixture with a solvent.

24. The process of claim 23, wherein the solvent is methanol or acetone.

25. The process of claim 21, wherein step b) is performed at a temperature below −100° C.

26. A process for making the solid dispersion of any one of claims 1-9, comprising:

a) obtaining a solid mixture of rasagiline or the pharmaceutically acceptable salt thereof, and the at least one polymeric pharmaceutical excipient; and

b) grinding the mixture.

27. The process of claim 26, wherein the pharmaceutically acceptable salt of rasagiline is rasagiline citrate.

28. The process of claim 27, wherein the rasagiline citrate is mono-rasagiline citrate.

29. The process of any one of claims 26-28, wherein step b) is performed by dry milling the mixture.

30. The process of claim any one of claims 26-28, wherein step b) is performed by wet milling the mixture with a solvent.

31. The process of claim 30, wherein the solvent is methanol or acetone.

32. The process of claim any one of claims 26-28, wherein step b) is performed at a temperature below −100° C.

33. A method of treating a human subject afflicted with Parkinson's disease comprising administering to the human subject an amount of the pharmaceutical composition of claim 10, effective to treat the human subject.