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The Effect of VSL#3 Probiotic Preparation on the Bile Acid Metabolism in Patients With Inflammatory Bowel Disease

Not Applicable
Active, not recruiting
Conditions
Crohn Disease
Ulcerative Colitis
Interventions
Dietary Supplement: VSL#3 (Original De Simone formulation)
Registration Number
NCT01765439
Lead Sponsor
Charles University, Czech Republic
Brief Summary

The aim of the study is to determine, whether administration of VSL#3 (Original De Simone formulation) probiotic preparation can alter the bile acid metabolism in patients with inflammatory bowel disease.

Detailed Description

VSL#3 (Original De Simone formulation, further abbreviated as VSL#3), a potent probiotic preparation, has been tested as an adjuvant therapy in inflammatory bowel diseases (IBD), chronic unspecific inflammatory disorders of the gastrointestinal tract (the most frequent forms of IBD are Crohn's disease (CD) and ulcerative colitis (UC)). VSL#3 has been shown to improve symptoms of IBD both in animal models and in humans-the most impressive results have been observed in preventing of pouchitis in UC patients. Several possible mechanisms of its action have been suggested, including change in gut microbial diversity, immunomodulatory function (upregulation of interleukine-10), etc., however, the list is probably far from complete.

Bile acids (BA) play an important role in the gastrointestinal tract - besides facilitating fat (and protein) digestion and resorption, they act as general antimicrobial agents within the small intestine (maintaining the small intestine more or less microbe-free), colonic microflora modifiers, intestinal innate immunity regulators, and importantly as signalling molecules on the liver-intestine/intestine-liver axis. Under pathological conditions (such as BA malabsorption) BA can worsen the IBD symptoms (namely diarrhoea), by irritating colonic mucosa or by inducing colonic secretion of electrolytes.

The study hypothesis is that the beneficial effect of VSL#3 might be partially explained by alteration of BA metabolism. There exists a complex crosstalk between gut microflora and BA: BA affect microbial growth, whereas BA structure is modified by bacteria (deconjugation, 7 α dehydroxylation). Several observations might support this hypothesis: VSL#3 ameliorates symptoms of radiation or chemotherapy induced diarrhoea, as well as diarrhoea of critically ill patients - conditions, that can be caused by BA malabsorption. Similarly, oxalate absorption (closely related to BA malabsorption) has been shown to be lowered by VSL#3. The main question to be addressed in the proposed study is, therefore, whether VSL#3 administration can somehow change metabolism of bile acids (BA).

Additionally, urinary metabolite levels are strongly influenced by differences in the intestinal microbiota, since both gut bacterial metabolism, and shared metabolism by the host and bacterial species ('co-metabolism'), generate specific metabolic products. Such metabolites may therefore be used as markers of microbial metabolic activity, reflecting systemic, functional differences. This application of urinary metabolic profiling avoids the technical difficulties, and methodological differences, found in molecular studies of the intestinal microbiota in IBD, which have contributed to often discrepant findings. Specific urinary metabolites related to gut microbial metabolism differ between CD patients, UC patients, and controls. The emerging technique of urinary NMR-based metabolic profiling with multivariate analysis was able to distinguish these cohorts. This study should address the question, whether VSL#3 administration changes the nuclear magnetic resonance-based urinary metabolomic profile.

Recruitment & Eligibility

Status
ACTIVE_NOT_RECRUITING
Sex
All
Target Recruitment
79
Inclusion Criteria

Arm CD resected

  • confirmed diagnosis of Crohn´s disease (at least 6 months)
  • history of single resection of terminal ileum (at least 6 months before inclusion)
  • maximum length of resected ileum is 60 cm
  • no signs of disease activity (clinical, endoscopical, laboratory)
  • stable medication

Arm UC unoperated

  • confirmed diagnosis of ulcerative colitis (at least 6 months)
  • no signs of disease activity (clinical, endoscopical, laboratory)
  • stable medication

Arm UC IPAA

  • confirmed diagnosis of ulcerative colitis (at least 6 months)
  • proctocolectomy and IPAA (at least 3 months before inclusion)
  • no signs of disease activity (clinical, endoscopical, laboratory)
  • stable medication

Arm Healthy volunteers

  • no signs of gastrointestinal disorder
  • initial laboratory examination within normal range (blood count, liver function tests, C-reactive protein, Fe, ferritin, fecal calprotectin)
Exclusion Criteria
  • use of bile acids
  • use of bile acids sequestrants
  • use of farnesoid X receptor agonists/antagonists
  • recent colonoscopy(less than 1 month before inclusion)
  • diabetes

Study & Design

Study Type
INTERVENTIONAL
Study Design
PARALLEL
Arm && Interventions
GroupInterventionDescription
Healthy volunteersVSL#3 (Original De Simone formulation)Subjects without any sign of disease of the digestive tract.
CD resectedVSL#3 (Original De Simone formulation)Patients with Crohn´s disease with the history of single resection (\<60 cm) of distal leum.
UC unoperatedVSL#3 (Original De Simone formulation)Patients with ulcerative colitis without history of gut resection.
UC IPAAVSL#3 (Original De Simone formulation)Patients with ulcerative colitis after proctocolectomy and ileal pouch-anal anastomosis(IPAA).
Primary Outcome Measures
NameTimeMethod
Alteration in the rate of bile acid synthesisBaseline and 6 weeks (plus or minus 5 days)

Will be assessed as difference between serum levels of fibroblast growth factor 19 and C4 at baseline and 6 weeks, respectively.

Secondary Outcome Measures
NameTimeMethod
Change of a metabolomic profile in urineBaseline and 6 weeks (plus or minus 5 days).
Change of the spectrum of bile acids in stools and plasmaBaseline and 6 weeks (plus or minus 5 days).

Related Research Topics

Explore scientific publications, clinical data analysis, treatment approaches, and expert-compiled information related to the mechanisms and outcomes of this trial. Click any topic for comprehensive research insights.

What molecular mechanisms does VSL#3 use to alter bile acid deconjugation and 7α dehydroxylation in IBD patients?
How does VSL#3's effect on bile acid metabolism compare to anti-TNF agents in IBD patients?
Which urinary metabolomic biomarkers correlate with VSL#3-induced changes in bile acid metabolism for UC and CD patients?
What are the known adverse events of VSL#3 administration in IBD patients and how are they managed?
Are there other probiotics or combination therapies that modulate bile acid metabolism similarly to VSL#3 in IBD?

Trial Locations

Locations (1)

Iscare I.V.F.

🇨🇿

Prague, Czechia

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