Clinical Trial Details
— Status: Completed
Administrative data
| NCT number |
NCT02865707 |
| Other study ID # |
Pro00041938 |
| Secondary ID |
|
| Status |
Completed |
| Phase |
N/A
|
| First received |
|
| Last updated |
|
| Start date |
August 2016 |
| Est. completion date |
December 2020 |
Study information
| Verified date |
March 2020 |
| Source |
University of Alberta |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
Ulcerative colitis (UC) is a relapsing chronic intestinal inflammation with no existing cure,
that affects over 300 per 100.000 Canadians, the highest prevalence in the world. The
standard drug therapies are expensive and potentially toxic, and mostly directed against the
chronic inflammatory process. UC is the result of a dysbiosis between disease-inducing and
protective intestinal bacteria in a genetically susceptible host. Non-digestible dietary
carbohydrates (NDC) stimulate the growth of protective endogenous intestinal bacteria which
ferment them into short-chain fatty acids (SCFA), some of the latter with natural
anti-inflammatory properties, and are called prebiotics. The investigator was the first to
report that oral intake of NDC, the dietary β-fructans inulin plus fructo-oligosaccharides
(FOS), reduced colitis in a genetically-induced rat colitis model. Both inulin and FOS
reduced colitis, each NDC modifying specific luminal microbiota. A small trial with the same
mixture of NDC in patients with active UC relapsing on oral 5-aminosalicylic acid (5-ASA)
showed a dose-dependent clinical response, confirming the translational potential of this NDC
mixture.
The investigators propose a randomized placebo-controlled trial to assess if inulin plus FOS
can also prevent such relapses in UC patients with inactive disease on stable maintenance
drugs. Primary hypothesis is that inulin plus FOS is effective adjunct therapy to standard
drugs for maintaining clinical remission. The second hypothesis is that the colonic
microflora and its metabolic function, altered by inulin plus FOS, or not, mediate protection
or relapse in UC. The longitudinal design of this maintenance prevention study and by
serially collecting colon biopsies, stool, serum and urine within the same patient before a
relapse (inflammation) occurs, would enable to identify unique changes in the intestinal
microbiota, their metabolic functions and also assess effects on host-immune response that
are associated with remission or before a relapse occurs during treatment with beta-fructans,
or not.
Description:
Objectives: Based on the efficacy of inulin plus FOS shown in experimental colitis as well as
their ability to improve active human UC the investigators propose double-blind placebo
controlled study using Synergy1, a 1:1 FOS/ inulin mixture, in patients in clinical remission
of UC. The specific aims of this study are as follow:
1. To determine if β-fructans are effective in maintaining clinical remission in UC
patients.
2. To examine the mechanisms of action of β-fructans on the intestinal microbiota
composition and function and host immune response of these patients.
It is hypothesized that β-fructans will prolong remission in UC patients with inactive
disease maintained on standard drug therapy and that the prebiotics beneficial effect is
associated with enhanced colonic energy homeostasis as a result of specific stimulation of
butyrate- and/ or other SCFA-producing microorganisms combined with improved host mucosal
energy and inflammation regulation.
The proposed trial
Trial Design: A double blind placebo controlled clinical trial
Intervention and duration of treatment: All patients in the treatment group will receive
chicory-derived β-fructans inulin plus FOS (1:1) ("Synergy1") for 6 months. Synergy1 will be
administered as 7.5 gram dose twice a day as a pre-packaged powder added to meals and
provided by Beneo-Orafti. This 15 gram daily prebiotic dose was found to be most effective in
treating mild to moderately active UC in the investigator's previous pilot study. Patients in
the placebo group will receive non-fermentable maltodextrin with a similar appearance, dosage
and frequency as β-fructans. Patients that completed the 6 months treatment period will be
monitored for disease related symptoms for additional 6 months.
Co-Intervention: Participants will continue at standard maintenance therapy for the duration
of the trial. Participants will be asked to maintain their regular diet. This will be
confirmed by having subjects complete the Food Frequency Questionnaire and assessing dietary
intake at 0 and 6 months of the study, or at relapse, using online system. Compliance will be
assessed by counts of study agent packages and by metabolomic analysis of participants serum
and urine.
Specimen Samples: Fecal samples will be collected for fecal calprotectin (FC) and microbiota
analysis at 0, 1, 3, 6 and 12 months, or at relapse. Colon biopsies will be collected between
15-20 cm from the anus for host mucosal response (4 biopsies), microbiota studies (4
biopsies) and histology (2 biopsies) at the start, and at 6 months, or at relapse. Urine and
blood/serum will be collected for metabolomics analysis at 0, 1, 3 and 6 month of treatment,
or at relapse. Colonic luminal washes will be collected at the start and at 6 months or at
relapse during the sigmoidoscopy exam.
Sample Size: Ninety patients, 45 in each arm, will be needed to detect a difference of 30 %
in the proportion of UC patients with clinical recurrence by 6 months with a power of 80%
using a two-sided p=0.05 level test. An anticipated dropout rate for this trial will be 10%,
based on previous maintenance trials, therefore the overall sample size for this trial will
be 100 patients.
Outcomes:
Primary Outcome: The proportion of patients with relapse over 6 months. Relapse is defined as
an increase of Mayo score of 3 or more with an endoscopy grade equal to or more than 2, and
rectal bleeding for at least 3 days. The relapse rate in the prebiotic-treated group at 6
month will be compared to the relapse rate in the placebo group.
Secondary outcomes: 1) Time to relapse. 2) Patient compliance and tolerability. Compliance
will be assessed as a ratio of packages (used) divided by the total packages dispensed over 6
months. Tolerability will be assessed by a validated questionnaire by Casellas et al on
adverse effects such as bloating and flatulence, compliance by package, pill counting and
metabolomic analysis at 3 and 6 months, or at relapse. 3) Intestinal inflammation (measured
by fecal calprotectin) at baseline and months 1, 3 and 6, or at relapse. 4) Microscopic
inflammation scores (0 and 6 months, or at relapse)
Basic science parameters: 1) Colonic biopsies for cytokine measurement, butyrate transporters
and oxidation pathway and Mucin 2 (MUC2) mRNA expression analysis, histological assessment
and characterization and quantification of the mucosa-associated microbiota; 2) Stool and
urine for assessment of fecal calprotectin concentrations, the luminal microbiota and its
metabolic products using pyrosequencing, quantitative PCR (qPCR) and gas chromatography (GC)
and nuclear magnetic resonance (NMR); 3) Blood/serum for metabolomic analysis with GC and
NMR; 4) colonic luminal wastes for assessing the Immunoglobulin G (IgG) associated
microbiota.
