FAECALIBACTERIUM PRAUSNITZII STRAINS FOR TREATING AND PREVENTING GASTROINTESTINAL PAIN
The present invention relates to a bacterial strain of the Faecalibacterium prausnitzii species selected from a bacterial strain belonging to one of the phylogroups I, II and III, for use in the treatment and/or prevention of visceral abdominal pain in an individual. The present invention also concerns compositions comprising said bacterial strains as well as specific strains as such.
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The present invention concerns Faecalibacterium prausnitzii strains for use in the treatment and prevention of visceral abdominal pain in an individual, in particular of gastrointestinal pain of non-inflammatory origin.
The present invention also concerns a composition, in particular an oral composition, comprising specific Faecalibacterium prausnitzii strains as well as new Faecalibacterium prausnitzii strains per se.
PRIOR ARTVisceral abdominal pain, and in particular gastrointestinal pain, is a very common disorder that affects millions of people every year all over the world and is a leading cause of patient visits to clinics. Abdominal pain is present on questioning of 75 percent of otherwise healthy adolescent students (Hyams et al. J. Pediatr. 1996; 129:220) and in about half of all adults (Heading; Scand J Gastroenterol Suppl. 1999; 231:3).
Such visceral pain can originate from various origins such as peptic disease, pancreatitis in alcoholics, inflammatory bowel disease, appendicitis, ruptured viscus, acute volvulus or even gastritis, biliary colic, gastroenteritis, splenic rupture, hepatic laceration or small bowel rupture.
However, gastrointestinal disorders, in particular non-inflammatory gastrointestinal disorders, and more particularly Irritable Bowel Syndrome (IBS), are the most frequent reasons for visceral abdominal pain in an individual.
IBS is one of the 25 most wide-spread recognized pathologies of the gastrointestinal tract. In the USA and in the first five European countries (France, Germany, the United Kingdom, Spain and Italy), in 2009, IBS affected more than 24 million persons. IBS accounts for 40 to 60% of referrals to gastroenterology outpatient clinics (Jones et al., Gut 2000; 47(Suppl 2): ii1-ii19).
Three subgroups of IBS patients have been defined based on the predominant bowel habit: constipation-predominant (c-IBS), diarrhea-predominant (d-IBS) or alternating between 25 the two (a-IBS). The definition and diagnostic criteria for IBS have been formalized in the “Rome Criteria” (Drossman et al. 1999, Gut 45:Suppl II: 1-81).
The pathophysiology of IBS is believed to involve alterations in the brain-gut axis. However, the mechanisms by which these changes lead to IBS remain poorly understood.
IBS is in particular characterized by a colonic hypersensitivity. This pain sensitivity is usually studied using variation of balloon distention in the rectum, a procedure in which a balloon is inserted into the rectum and slowly inflated. This common complaint is a crucial feature because of its significant impact on a patient's quality of life and lack of efficient therapies.
However, the current treatments against IBS and visceral abdominal pain are disappointing.
There is thus a need for new substances, in particular probiotics, or compositions for the treatment and/or prevention of visceral abdominal pain, in particular gastrointestinal pain, in an individual.
There is also a need for new substances, in particular probiotics, or compositions for preventing and/or treating visceral abdominal pain in an individual suffering from a non-inflammatory gastrointestinal disorder, in particular from an Irritable Bowel Syndrome (IBS).
More particularly, there is a need in the prior art for new substances, in particular probiotics, or compositions that are able to diminish the sensitivity of nociceptors in the gastrointestinal tract of an individual, in particular in individuals suffering from a colonic hypersensitivity.
SUMMARY OF THE INVENTIONThe present invention aims to provide novel substances, in particular probiotics, and compositions for treating and/or preventing visceral abdominal pain in an individual, more particularly gastrointestinal pain of non-inflammatory origin.
According to the inventors' experimental results, specific Faecalibacterium prausnitzii (F. prausnitzii) strains, belonging to three particular phylogroups previously described (Lopez-Siles et al., 2012), possess the unexpected ability to diminish visceral abdominal pain in an individual. As illustrated in the Examples and discussed further, the inventors have demonstrated that F. prausnitzii strains outside of these phylogroups, such as the strain CNCM I-4541, do not possess such advantageous properties.
The properties of the F. prausnitzii strains of the invention have been demonstrated in the examples by the inventor's in two different models: a Neonatal Maternal Separation (NMS) colonic hypersensitivity (CHS) mouse model and a Partial Restraint Stress (PRS) rat model.
Strains according to the invention are more particularly able to diminish the sensitivity of nociceptors in the gastrointestinal tract of an individual and consequently to prevent and/or reduce colonic hypersensitivity of said individual.
According to a first object, the present invention relates to a bacterial strain of the Faecalibacterium prausnitzii species selected from a bacterial strain belonging to one of the phylogroups I, II and III according to the invention, for use in the treatment and/or prevention of visceral abdominal pain in an individual.
These strains identified by the inventors are thus probiotics that can be used for the above-indicated purposes.
An individual according to the invention is a mammal, in particular a human.
Visceral abdominal pain is pain associated with organs of the abdomen of the individual.
The visceral abdominal pain is in particular a gastrointestinal pain, in particular a colonic pain.
A bacterial strain of the Faecalibacterium prausnitzii species according to the invention is different from the strain A2-165.
According to a preferred embodiment, bacterial strains according to the invention for use as indicated here above are selected from the group consisting of bacterial strains deposited to the CNCM under the accession numbers I-4542, I-4544, I-4540, I-4574, I-4543, I-4575, I-4573, I-4644 and I-4546, and in particular the bacterial strain deposited to the CNCM under the accession number I-4573.
According to an embodiment, the visceral pain according to the invention is caused by a gastrointestinal disorder, in particular a non-inflammatory gastrointestinal disorder.
A gastrointestinal disorder of the invention, in particular according to this embodiment, can be a gastrointestinal hypersensitivity, in particular a colonic hypersensitivity, and is preferably an Irritable Bowel Syndrome, in particular an alternating-type Irritable Bowel Syndrome.
In particular, such gastrointestinal disorder according to the invention can be selected from the group consisting of IBS and constipation.
According to another embodiment, a bacterial strain for use according to the invention is comprised in a composition comprising a physiologically acceptable medium, preferably in an oral composition, and most preferably in a food supplement.
Thus, according to another object, the present invention relates to a composition comprising, in a physiologically acceptable medium, at least one bacterial strain of Faecalibacterium prausnitzii selected from the group consisting of bacterial strains deposited to the CNCM under the accession numbers I-4542, I-4544, I-4540, I-4574, I-4543, I-4575, I-4573, I-4644 and I-4546.
In a preferred embodiment, said bacterial strain of the Faecalibacterium prausnitzii species is the bacterial strain deposited to the CNCM under the accession numbers I-4573.
The term “physiologically acceptable medium” is understood to mean a medium that is compatible with the organism of the individual to whom said composition is intended to be administered. It can for example be any non-toxic solvent such as water. In particular, said medium is compatible with an oral administration.
A composition of the invention is preferably for the oral route and in particular in the form of a food supplement.
A composition of the invention for the oral route can be selected from the group consisting of a food product, a drink, a pharmaceutical, a nutraceutical, a food additive, a food supplement and a dairy product. It can in particular be a food supplement.
The inventors have also indentified new Faecalibacterium prausnitzii strains having the specific abilities discussed previously.
Consequently, a further object of the invention consists in an isolated bacterial strain selected from the group consisting of bacterial strains deposited to the CNCM under the accession numbers I-4542, I-4544, I-4540, I-4574, I-4543, I-4575, I-4573, I-4644 and I-4546.
According to a preferred embodiment, said bacterial strain is the bacterial strain deposited to the CNCM under the accession number I-4573.
As demonstrated in the examples, a Faecalibacterium prausnitzii strain of the invention has no negative impact in an individual not suffering from visceral abdominal pain according to the invention and is thus perfectly safe for use.
For illustrative purposes, Faecalibacterium prausnitzii strains CNCM I-4541 (SEQ ID No: 16) and 513E3 (SEQ ID No: 17) are outside the three phylogroups of the invention. The method for obtaining said distribution is discussed further below.
The present inventors have performed a huge amount of work with the view of identifying the ability of specific Faecalibacterium prausnitzii strains to treat and/or prevent visceral abdominal pain, and in particular gastrointestinal pain, in an individual.
The inventors have indeed unexpectedly determined that Faecalibacterium prausnitzii strains belonging to three phylogroups defined further exhibit the ability to diminish the sensitivity of nociceptors in the gastrointestinal tract of an individual.
The bacterial strains according to the invention can prevent and/or reduce visceral abdominal pain, in particular gastrointestinal pain, in an individual, in particular in an individual suffering from a gastrointestinal non-inflammatory disorder, and in particular from a colonic hypersensitivity, such as in IBS.
It is demonstrated herein that bacterial strains of the invention are in particular able to reduce the Vicero Motrice Response (VMR) of a colon when a balloon inserted into the rectum is slowly inflated in an IBS mouse model pre-treated with a bacterial strain of the invention. Said VMR is brought back to a normal intensity, since the VMR level observed after administration of a strain according to the invention is similar to the VMR observed in mice not suffering from colonic hypersensitivity.
Faecalibacterium prausnitzii Strains of the Invention
F. prausnitzii is a major member of the Firmicutes phylum and is part of the most abundant commensal bacteria in the healthy human large intestine microbiota. F. prausnitzii is an extremely oxygen sensitive (EOS) bacterium and is thus difficult to cultivate, even in anaerobic conditions (Duncan et al. 2002, Int. J. Syst. Evol. Microbiol. 52(Pt 6): 2141-6 and Lopez-Siles et al. Appl. Environ Microbiol. 2012 January;78(2):420-8). F. prausnitzii is in particular known as being one of the most abundant butyrate-producing bacterium in the human gastrointestinal tract, the short chain fatty acid butyrate being very important in gut physiology, systemic functions and beneficial effects for human health (Macfarlane and Macfarlane (2011), J. Clin. Gastroenterol. 45 Suppl: S120-7).
F. prausnitzii is also known for having anti-inflammatory and protective effects in murine models of acute and chronic colitis, i.e. in inflammatory disorders (Martin et al., Inflamm Bowel Dis. 2014 March; 20(3):417-30 and Sokol et al., Proc Natl Acad Sci USA. 2008 Oct. 28;105(43):16731-6).
Recently, diminished prevalence and abundance of F. prausnitzii have been reported in non-inflammatory intestinal disorders. A negative correlation has indeed been observed between the abundance of F. prausnitzii bacteria and IBS symptoms, in particular in alternating-type IBS.
Emerging evidences suggest that perturbation of the gastrointestinal microbiota, and in particular dysbiosis, plays a role in the pathophysiology of IBS (Ringel and Maharshak, Am. J. Physiol. Gastrointest. Liver Physiol. 2013 Oct. 15; 305(8): G529-41).
The ability of the F. prausnitzii strains of the invention to prevent visceral abdominal pain, and in particular gastrointestinal pain, in an individual is specific to the strains identified by the inventors, and constituting the three phylogroups of the invention.
Such specific antinociceptive activity is illustrated in the examples, wherein a comparative test has been performed with a F. prausnitzii strain not part of the three phylogroups of the invention, i.e. the strain CNCM I-4541. As demonstrated in these examples, this strain does not possess the antinociceptive activity of the strains of the invention.
Method for Obtaining Phylogroups of the Invention
Isolated Faecalibacterium prausnitzii strains have been classified by the inventors in three phylogroups illustrated in
Full-length 16S rRNA gene sequences of each strain were obtained or determined and compared one to the other.
Full-length 16S rRNA sequences of 17 F. prausnitzii strains are indicated as sequences SEQ ID No: 1 to 17.
DNA was extracted from isolated colonies of the different F. prausnitzii strains by alkaline lysis in 50 μL of NaOH 0.5 M during 30 min and 50 μl of Tris 1M pH7 and 100 μL H2O were added.
16S rRNA sequences were amplified and PCR products purified with the Wizard SV Gel. PCR Clean-Up system (Promega) was used to obtain bidirectional partial 16S rRNA gene sequences by using primers. All DNA sequences were confirmed by sequencing (Eurofins MWG Operon, Ebersberg, Germany).
Multiple sequence alignment was performed with hierarchical clustering for 16S rRNA gene sequence full-length construction (http://multalin.toulouse.inrafr/multalin) (COrpet F., Nucleic Acids Res. 1988; 16:10881-10890).
Phylogenetic analysis of the 16S rRNA gene was then performed using MEGA6 software package (http://www.megasoftware.net/). The evolutionary history was inferred using the Neighbor-Joining method (Saitou N. and Nei M., Mol Biol Evol. 1987; 4:406-425).
The optimal tree with the sum of branch length=0.24930207 is shown in
The tree is drawn to scale, with branch lengths in the same units as those of the evolutionary distances used to infer the phylogenetic tree. The evolutionary distances were computed using the Maximum Composite Likelihood method (Tamura et al., Proc Natl Acad Sci USA. 2004; 101:11030-11035) and are in the units of the number of base substitutions per site.
The analysis involved 35 nucleotide sequences. Codon positions included were lst+2nd+3rd+Non-coding. All positions containing gaps and missing data were eliminated.
There were a total of 1091 positions in the final dataset.
Eubacterium desmolans was used to root the tree (SEQ ID No: 18). In sequence SEQ ID No: 18, ‘n’ is used to represent any ambiguous nucleotides.
In order to verify if a given F. prausnitzii strain can be classified in one of the phylogroups I to III according to the invention, its 16S rRNA sequence needs to be compared through the MEGA6 software package discussed here-above directly to the one of the present invention.
According to an embodiment, a bacterial strain of the invention is selected from phylogroup I.
Bacterial strains belonging to phylogroup I can be represented by the strains consisting of:
-
- bacterial strains deposited to the CNCM under the accession numbers I-4542, I-4544 and I-4540; and
- bacterial strains of reference HTF-75H, S13A7, S3G1, L2-15, L2-39, L2-61 and L2-6.
Preferably, a bacterial strain belonging to phylogroup I is selected from the group consisting of bacterial strains deposited to the CNCM under the accession numbers I-4542, I-4544 and I-4540.
According to an embodiment, a bacterial strain of the invention is selected from phylogroup II.
Bacterial strains belonging to phylogroup I1 can for example be selected from the group consisting of bacterial strains of reference HTF-60C, HTF-I, HTF-E, HTF-C, HTF-A, HTF-B and HTF-F.
According to an embodiment, a bacterial strain of the invention is selected from phylogroup III.
Bacterial strains belonging to phylogroup III can be represented by the strains consisting of:
-
- bacterial strains deposited to the CNCM under the accession numbers I-4574, I-4543, I-4575, I-4573, I-4644 and I-4546; and
- bacterial strains of reference S3C12, S9G3, S9D8, S3L/3, S4L/4, M21/2 and S10H3,
with the proviso that the bacterial strain is different from the bacterial strain A2-165.
Preferably, a bacterial strain belonging to phylogroup III is selected from the group consisting of bacterial strains deposited to the CNCM under the accession numbers I-4574, I-4543, I-4575, I-4573, I-4644 and I-4546.
Bacterial strains of reference ATCC 27768, A2-165, L2-15, L2-39, L2-6, L2-61, M21/2, S3L/3, S4L/4, HTF-A, HTF-B, HTF-C, HTF-E, HTF-F, HTF-I, HTF-60C and HTF-75H can be obtained as indicated in Lopez-Siles et al., Appl. Environ. Microbiol. 2012, 78(2):420.
In a preferred embodiment, a bacterial strain of the invention is selected from phylogroups I and/or III. More particularly, a bacterial strain of the invention is selected from phylogroups I and/or III with the proviso that the bacterial strain is different from the bacterial strain A2-165.
According to an embodiment, a bacterial strain of the invention is selected from the group consisting of bacterial strains deposited to the CNCM under the accession numbers I-4542, I-4544, I-4540, I-4574, I-4543, I-4575, I-4573, I-4644 and I-4546.
A bacterial strain of the invention is preferably the bacterial strain deposited to the CNCM under the accession number I-4573.
The inventors have also indentified new Faecalibacterium prausnitzii strains having the specific abilities discussed previously.
Consequently, the present invention further concerns an isolated bacterial strain selected from the group consisting of bacterial strains deposited to the CNCM under the accession numbers I-4542, I-4544, I-4540, I-4574, I-4543, I-4575, I-4573, I-4644 and I-4546.
Said bacterial strain is in particular the bacterial strain deposited to the CNCM under the accession number I-4573.
A suitable daily dose of a bacterial strain according to the invention is from 103 to 1012 colony forming units (cfu), more preferably from 107 to 1011 cfu as a medicament, for example as a daily dose equivalent to 1010 cfu.
A Faecalibacterium prausnitzii strain of the invention is for use in the treatment and/or prevention of visceral abdominal pain in an individual.
The strains of the invention are probiotics whose activity lies in the gut. A probiotic bacterium according to the invention denotes a bacterium which ingested live in adequate quantities can exert beneficial effects on the human health.
These strains consequently need to be administered alive to the gut.
The bacteria strains of the invention can be administered to the gut of an individual to be treated by different ways, i.e. by the oral, rectal or parenteral route. A bacterium according to the invention is preferably administered by the oral or rectal route, more preferably by the oral route.
According to a preferred embodiment, a bacterial strain of the invention is comprised in a composition comprising a physiologically acceptable medium. Such composition is preferably for the oral route, and in particular in the form of a food supplement.
Compositions
The present invention further concerns a composition comprising, in a physiologically acceptable medium, at least one bacterial strain of Faecalibacterium prausnitzii of the invention.
More particularly, according to an embodiment, the present invention relates to a composition comprising, in a physiologically acceptable medium, at least one bacterial strain of Faecalibacterium prausnitzii selected from the group consisting of bacterial strains deposited to the CNCM under the accession numbers I-4542, I-4544, I-4540, I-4574, I-4543, I-4575, I-4573, I-4644 and I-4546.
Preferably, a composition according to the invention comprises at least one bacterial strain deposited to the CNCM under the accession number I-4573.
A composition according to the invention is intended for the gastrointestinal tract, in particular the gut.
Consequently, a composition according to the invention is selected from an oral, rectal or parenteral composition. A composition of the invention is preferably an oral or rectal composition, more preferably an oral composition.
According to an embodiment, a composition of the invention is an oral composition, i.e. is intended for oral administration to a subject.
Such composition can be in the form of a suspension, tablet, pill, capsule, granulate or powder.
The composition according to the invention for the oral route can be selected from the group consisting of a food product, a drink, a pharmaceutical, a nutraceutical, a food additive, a food supplement or a dairy product, and is in particular a food supplement.
According to a preferred embodiment, a composition according to the invention is a food supplement.
Food supplement for oral administration may be present in capsules, gelatin capsules, soft capsules, tablets, sugar-coated tablets, pills, pastes, pastilles, gums, drinkable solutions or emulsions, a syrup or a gel.
Advantageously, a composition according to the invention, intended for oral administration, can be provided with a coating resistant to gastric juice, so as to ensure that the bacterial strain of the invention comprised in said composition can pass through the stomach undamaged. The release of the bacterial strain can thus takes place for the first time in the upper intestinal tract.
A food supplement according to the invention can also include a sweetener, a stabilizer, an antioxidant, an additive, a flavouring agent and/or a colorant.
The formulation thereof is carried out by means of the usual methods for producing sugar-coated tablets, gel capsules, gels, hydrogels for controlled release, emulsions, tablets or capsules.
A composition according to the invention can also be in the form of a nutritional composition.
A nutritional composition according to the invention is in the form of a yogurt, a cereal bar, a breakfast cereal, a dessert, a frozen food, a soup, a pet food, a liquid suspension, a powder, a tablet, a gum or a candy.
In a further embodiment of the invention, a composition containing a bacterial strain of the invention is administered intrarectally.
A rectal administration preferably takes place in the form of a suppository, enema or foam.
A composition according to the invention contains an amount of bacterial strains of the invention equivalent to between 103 and 1012 cfu/g (dry weight basis), more preferably between 106 and 109 cfu/g.
A composition according to the invention can further comprise at least one of: antioxidants, fish oils, DHA, EPA, vitamins, minerals, phytonutrients, protein, fat, probiotics, and combinations thereof.
The present invention further concerns the use of at least one bacterial strain of the Faecalibacterium prausnitzii species selected from a bacterial strain belonging to at least one of the phylogroups I, II and III, for the treatment and/or prevention of visceral abdominal pain in an individual.
The present invention also concerns the use of a composition, preferably an oral composition, comprising, in a physiologically acceptable medium, at least one bacterial strain of the Faecalibacterium prausnitzii species selected from a bacterial strain belonging to at least one of the phylogroups I, II and III, for the treatment and/or prevention of visceral abdominal pain in an individual.
The invention will be described below in greater details using the following examples which are given for illustrative purposes only.
All references to percentages are percentages by weight unless otherwise stated.
EXAMPLESF. prausnitzii strains according to the invention have been tested for their ability to have a direct impact on visceral pain, and more particularly on colonic hypersensitivity.
Bacterial Strains Isolation and Growth Conditions
The F. prausnitzii strains isolates used in the present example all are of human fecal origin from healthy patients. Said isolates were obtained from the highest countable dilution of human fecal samples in roll tubes of anaerobic M2GSC medium as discussed in Lopez-Sites et al. (Appl. Environ Microbiol. 2012; 78:420-428).
Tested F. prausnitzii strains isolates were grown in LYBHI medium (Brain-Heart infusion medium supplemented with 0.5% yeast extract) (Dyfco, Detroit, USA) supplemented with 1 mg/mL cellobiose (Sigma-Aldrich Chemie Gmbh, Buchs, Switzerland), 1 mg/mL maltose (Sigma-Aldrich) and 0.5 mg/mL cysteine (Sigma-Aldrich) at 37° C. in anaerobic chamber.
A. In a first series of tests, a Neonatal Maternal Separation (NMS) colonic hypersensitivity (CHS) mouse model is used.
a. NMS CHS Mouse Model
Pregnant C57Bl/6J mice have been purchased from Janvier laboratories (Le Genest Saint Isle, France).
After birth, wild-type C57Bl/6J were isolated from their mother from D2 to D14, three hours a day, from 9 a.m. to 12 a.m. At nine-week old age, male mice were orally treated each day for nine days with 200 μL of 10×1010 CFU/mL of:
-
- the strain CNCM I-4573 according to the invention;
- the strain CNCM I-4541 outside the invention; or
- PBS as control.
All the experiments were performed on the last day of treatment at D10.
The same bacteria treatment was administered to non-NMS CHS mice as a control.
NMS treatment induced an increased Vicero Motrice Response (VMR) in the absence of any significant alteration in gut wall macroscopic integrity or colonic mucosa inflammation (Coutinho et al. (2002), Am. J. Physiol. Gastrointest. Liver Physiol. 282(2): G307-16).
As described in Christianson et al. 2007 (Nat Protoc 2(10): 2624-31), colonic sensitivity was assessed by quantifying visceromotor response with abdominal electromyography (EMG) recordings in response to colorectal distension.
The inventors also validated this model as being non-inflammatory by checking the cytokines pattern by measurement of 13 types of cytokines in serum samples of stressed (MS: Maternal separated) and non-stressed (NH: Non-handled) mice.
It was observed that there are no differences in cytokine pattern induced by the chronic stress.
Moreover, NMS does not induce changes in colonic macroscopic damage, loss of architectural epithelium, goblet cell depletion, oedema/ulceration or inflammatory cell infiltrates.
Furthermore, NMS does not induce changes in body weight, colon weight and length and in spleen weight when stressed (MS) mice are compared to the control group (PBS).
b. Statistical Analysis
Statistical analysis was completed using GraphPad software (GraphPad Software, La Jolla, Calif., USA). All data were expressed as mean+/−SEM.
MS mice displaying VMR values lower than mean minus two SEM for all distension volumes were considered as non-sensitized and excluded from the analysis.
For VMR analysis in model validation, a two-way (Volume & Treatment) ANOVA followed by Bonferroni post-hoc test for multiple comparisons was used.
P<0.05 was considered statistically significant.
c. Results
The results obtained are presented in
As it can be seen in
More importantly, it can be seen that MS mice to whom CNCM I-4573 bacteria of the invention were administered possess a VMR statistically similar to the one of NH mice, all along the growth of the Volume Distension.
On the contrary, in
Treatment based on the administration of F. prausnitzii strain CNCM I-4573 according to the invention led to a specific and significant decrease of the VMR in the tested mice as well as a prevention of the increase of the VMR.
On the contrary, the treatments based on the control tests (NH mice) and on the administration of F. prausnitzii strain CNCM I-4541 present no effect on the VMR of all the tested mice.
The present results clearly demonstrate that F. prausnitzii strains according to the invention have a specific and unexpected beneficial effect on visceral abdominal pain.
B. In a second series of tests, a Partial Restreint Stress (PRS) rat model is used.
a. Partial Restraint Stress (PRS) Rat Model
Animal preparation was performed as previously described in Ait-Belgnaoui et al.; Gut 55, 1090-1094 (2006).
Briefly, under general anesthesia induced by i.p. administration of 0.6 mg/kg acepromazine (Calmivet, Vetoquinol, Lure, France) and 120 mg/kg ketamine (Imalgene 1000, Merial, Lyon, France), female Wistar rats (Rosztoczy, A. et al.; Neurogastroenterol. Motil. Off. J. Eur. Gastrointest. Motil. Soc. 15, 679-686 (2003)) were equipped with three groups of three NiCr wire electrodes (60 cm in length, 80 nm in diameter) implanted into the abdominal external oblique muscle, 2 cm above the inguinal ligament.
Electrodes were exteriorized at the neck level by a glass tube attached to the skin.
During the ten days previous to the stress, 1 ml of ±1×109 CFU or PBS were daily intragastrically administrated.
The study groups are as follows:
-
- the strain CNCM I-4573 according to the invention;
- the strain CNCM I-4541 outside the invention; or
- PBS as control.
All stress sessions were performed at the same time of the day (between 10 am and 12 pm) to minimize any influence of circadian rhythms. Stresses were performed using the wrap partial restrain stress model which is a mild non-ulcerogenic stressor (Williams, C. L et al.; Am. J. Physiol. 253, G582-586 (1987)).
Animals were lightly anesthetized (as previously described in Lee B. et al.; J. Neurogastroenterol. Motil. 17, 252-266 (2011), with ethyl-ether and their fore shoulders, upper forelimbs and thoracic trunk were draped in a confining harness of paper tape to restrict, but not to prevent, body movements.
Then rats were placed in their home cage for 2 h.
b. Rectal or Colorectal Distension and Colonic Hypersensitivity Measurement
Rats colonic sensitivity induced by PRS was assessed by quantifying electrical response through an electroencephalograph Reega Mini-hui (ALVAR, France) and expressed as number of abdominal cramps for a five min period (as previously described in Eutamene, H. et al.; J. Physiol. 506 (Pt 1), 245-252 (1998)).
Briefly, rats were accustomed to be in polypropylene tunnels (diameter 7 cm, length 20 cm) several days before colorectal distension (CRD) in order to minimize recording artifacts.
CRD was performed with an arterial embolectomy catheter (Fogarty; Edwards Laboratoire, Inc., Santa Ana, Calif., USA) introduced into the rectum (1 cm from the anus) and fixed at the base of the tail.
Distension of the colon was performed by connecting the catheter to a syringe and consecutive injections of different volumes (0.4, 0.8, 1.2 ml) with an interval of 5 minutes.
Each animal was recorded two days before the stress (basal measure) and just after the PRS (stress measure).
c. Statistical Analysis.
Statistical analysis was completed using GraphPad software (GraphPad Sofware, La Jolla, Calif., USA).
Results are presented with means±SEM.
Differences in the number of abdominal cramps during 5 minutes to gradual CRD volumes were analyzed using a 2-way ANOVA (Treatment, Volume) followed by Bonferroni post-hoc test for multiple comparisons.
A p value of less than 0.05 was considered significant.
d. Results
To determine if F. prausnitzii CNCMI-4541 (outside of the invention) and CNCMI-4573 (according to the invention) strains are able to prevent acute stress generated symptoms on visceral sensitivity, both were tested on a model of Partial Restraint Stress (PRS).
PRS increased the number of abdominal cramps in response to CRD in a volume-dependent manner (
In stressed rats treated with PBS, distensions at any volumes significantly increased the number of abdominal contractions compared to non-stressed animals (p<0.01) (
F. prausnitzii CNCMI-4573 strain treatment prevented this stress-induced visceral hypersensitivity until 0.8 ml distension volume (p<0.001) (
In basal conditions, no difference was observed in the VMR to CRD between the different treatments (
In contrast, F. prausnitzii CNCMI-4541 strain did not show a protective effect (
In conclusion, it appears that a F. prausnitzii strain according to the invention prevents visceral hypersensitivity in a model of Partial Restraint Stress (PRS).
Claims
1. A method of treating and/or preventing visceral abdominal pain in an individual, comprising
- administering to the individual a therapeutically effective amount of at least one Faecalibacterium prausnitzii bacterial strain belonging to phylogroup I, II and/or III.
2. The method according to claim 1, wherein the at least one Faecalibacterium prausnitzii bacterial strain belongs to phylogroup I and/or phylogroup III.
3. The method according to claim 1, wherein the at least one Faecalibacterium prausnitzii bacterial strain belongs to phylogroup I and is selected from the group consisting of bacterial strains deposited to the CNCM under accession numbers I-4542, I-4544 and I-4540.
4. The method according to claim 1, wherein the at least one Faecalibacterium prausnitzii bacterial strain belongs to phylogroup III and is selected from the group consisting of bacterial strains deposited to the CNCM under accession numbers I-4574, I-4543, I-4575, I-4573, I-4644 and I-4546.
5. The method according to claim 1, wherein the at least one Faecalibacterium prausnitzii bacterial strain is selected from the group consisting of bacterial strains deposited to the CNCM under the accession numbers I-4542, I-4544, I-4540, I-4574, I-4543, I-4575, I-4573, I-4644 and I-4546.
6. The method according to claim 1, wherein the visceral abdominal pain is a gastrointestinal pain.
7. The method according to claim 1, wherein the visceral abdominal pain is caused by a gastrointestinal disorder.
8. The method according to claim 7, wherein the gastrointestinal disorder is a gastrointestinal hypersensitivity.
9. The method according to claim 1, wherein the bacterial strain is comprised in a composition comprising a physiologically acceptable medium.
10. A composition comprising, in a physiologically acceptable medium, at least one bacterial strain of Faecalibacterium prausnitzii selected from the group consisting of bacterial strains deposited to the CNCM under the accession numbers I-4542, I-4544, I-4540, I-4574, I-4543, I-4575, I-4573, I-4644 and I-4546.
11. The composition according to claim 10, wherein the at least one bacterial strain of Faecalibacterium prausnitzii is the bacterial strain deposited to the CNCM under the accession number I-4573.
12. The composition according to claim 10, wherein the composition is for oral administration and is selected from the group consisting of a food product, a drink, a pharmaceutical, a nutraceutical, a food additive, a food supplement and a dairy product.
13. An isolated bacterial strain selected from the group consisting of bacterial strains deposited to the CNCM under the accession numbers I-4542, I-4544, I-4540, I-4574, I-4543, I-4575, I-4573, I-4644 and I-4546.
14. The isolated bacterial strain according to claim 13, being the bacterial strain deposited to the CNCM under the accession number I-4573.
15. The method of claim 5, wherein the at least one Faecalibacterium prausnitzii bacterial strain is a bacterial strain deposited to the CNCM under accession number I-4573.
16. The method of claim 6, wherein the gastrointestinal pain is a colonic pain.
17. The method according to claim 7, wherein the gastrointestinal disorder is a non-inflammatory gastrointestinal disorder.
18. The method according to claim 8, wherein the gastrointestinal hypersensitivity is a colonic hypersensitivity selected from Irritable Bowel Syndrome and alternating-type Irritable Bowel Syndrome.
19. The method according to claim 9, wherein the physiologically acceptable medium is a food supplement.
20. The composition of claim 12, wherein the composition is a food supplement.
Type: Application
Filed: Nov 13, 2015
Publication Date: Dec 19, 2019
Applicants: INSTITUT NATIONAL DE LA RECHERCHE AGRONOMIQUE (INRA) (Paris), INSTITUT NATIONAL DE LA SANTE ET DE LA RECHERCHE MEDICALE (INSERM) (Paris), UNIVERSITE PIERRE ET MARIE CURIE (PARIS 6) (Paris Cedex 05), ASSISTANCE PUBLIQUE - HOPITAUX DE PARIS (APHP) (Paris), ECOLE D'INGENIEURS DE PURPAN (Toulouse)
Inventors: Philippe LANGELLA (Velizy-Villacoublay), Sylvie MIQUEL (Beaumont), Rebeca MARTIN ROSIQUE (Jouy en Josas), Luis BERMUDEZ HUMARAN (Jouy en Josas), Muriel THOMAS (Igny), Harry SOKOL (Paris), Frédéric CARVALHO (Clermont-Ferrand), Vassilia THEODOROU (Portet Sure Garonne)
Application Number: 15/524,808