Irritable Bowel Syndrome With Diarrhea Clinical Trial
Official title:
A Study Evaluating the Effects of Low and High FODMAP Diets on Mucosal Protease Nerve Interactions in IBS Patients
OBJECTIVE: To gain mechanistic insights, we will compare effects of low fermentable
oligosaccharides, disaccharides and monosaccharides and polyols (FODMAP) and high FODMAP
diets on symptoms and colonic protease expression in patients with diarrhea predominant
irritable bowel syndrome (IBS-D). We will measure how protease changes affect excitability of
pain sensing neurons and correlate this with measurements of the metabolome and the
microbiome.
DESIGN: We aim to perform a single blind prospective study of patients with diarrhea
predominant IBS (Rome IV criteria) who will sequentially consume a high and low FODMAP diets,
each for 3 weeks. Symptoms will be assessed using the IBS symptom severity scoring (IBS-SSS).
Electrophysiological studies of changes in mouse dorsal root ganglia neurons in response to
colonic mucosal/lamina propria supernatants will be carried out. Protease antagonist will be
used to specifically assess protease expression. The metabolome will be evaluated using
metabolic profiling in urine using mass spectrometry. Stool microbiota composition will be
analysed by 16S rRNA gene profiling. All the above testing will be performed at 4 time
points: at baseline, 3 weeks following a run-in period, after a 3-week-long high FODMAP diet,
and after a 3-week-long low FODMAP diet period.
HYPOTHESIS: We anticipate that colonic tissue protease effects on the excitability of dorsal
root ganglia (DRG) neurons will increase with a high FODMAP diet and decrease with a low
FODMAP diet, but that this may not be found in all patients. The magnitude of the effect may
vary and this variation could be due to differences in the individual patients microbiome.
Up to 15 % of adults in Western society suffer from irritable bowel syndrome (IBS), and it is
the second leading cause, behind the common cold, of workplace absenteeism. This proposal
addresses critical knowledge gaps in our understanding of IBS mechanisms. What environmental
triggers cause pain symptoms to chronically wax and wane? A fundamental observation is that
over 70% of IBS patients report that meals trigger abdominal pain and diarrhea. Therefore, we
examined the effects of a diet low in fermentable oligo, di, monosaccharides and polyols
(FODMAPs) because up to 50-70% IBS patients reported improved symptoms on this diet (McIntosh
et al 2016; Halmos et al 2014). We found that symptoms, particularly pain, were markedly
improved in IBS patients on a low compared to a high FODMAP diet. Moreover, we found in a
subset of patients evidence that FODMAPs activate intestinal mast cells, a major source of
proteases and histamine, and their expression appears to be associated with IBS symptoms,
although this remains to be proven. Thus, this diet provides a useful clinical tool to
stimulate protease activity and study their actions. Sensitization (modulation of
intracellular mechanisms leading to exaggerated action potential discharge in response to a
given stimulus) of nociceptive dorsal root ganglia (DRG) neurons by tissue mediators is a
fundamental mechanism underlying abnormal pain signaling. We also have compelling evidence in
human IBS patients that a family of proteases are key mediators underlying another critical
knowledge gap that we identified, i.e. which tissue mediators can lead to sustained and
amplified abdominal pain. We and others found these proteases are elevated in IBS tissues,
and that they sensitize DRG neurons - the primary sensory neurons that innervate the colon.
Based on these findings, our goal is to test the overarching hypothesis that diet can trigger
recurrent symptoms in IBS through activation of tissue proteases that cause exaggerated pain
by signaling to nociceptive DRG neurons. Recurrent exposure to such diet components and the
resulting protease signaling is an important cause of the waxing and waning of symptoms over
time. Thus, our objective is to characterize the relationship of a specific dietary
intervention with protease activity in IBS patients.
This will be a prospective study comparing the effect of low-FODMAP and high-FODMAP on
symptoms and protease effects on the excitability of nociceptive DRG neurons. We will analyze
the urinary metabolome as a secondary measure of mast cell mediators (i.e. histamine and
proteases). We will also collect stool for possible future microbiome analysis as diet
microbiome interactions (i.e. fermentation of the FODMAPs) may predict the magnitude of the
response. The study will be conducted at Hotel Dieu Hospital's Gastroenterology clinics and
endoscopy suite in Kingston, Ontario. This study will be comprised of the following four time
periods: "baseline", "run-in", "high FODMAP diet", and "low FODMAP diet". Participants will
undergo baseline assessment with questionnaires on demographics, IBS symptoms (IBS symptom
severity scoring questionnaire), diet, as well as a questionnaire pertaining to psychological
parameters. A detailed questionnaire pertaining to participants' diet will be administered at
baseline. Baseline mucosal colonic biopsies will be obtained using limited flexible
sigmoidoscopy. Baseline stool microbiota composition will be analysed by 16S rRNA gene
profiling. Fecal calprotectin levels will be obtained from stool samples. Urine and blood
metabolome will be analysed at baseline also using mass spectrometry. These will be repeated
3 weeks later during a run-in period to assess if these measurements are stable in time or
not. This run-in period will be 3 weeks long. After completion of the run-in period, patients
will be asked to consume a high FODMAP diet for 3 weeks. All tests carried out at baseline
and during the run-in period will be carried out for a third time. Participants will meet
with investigators and be given dietary guidance, including a handout outlining foods to eat
and avoid. A dietician will be involved extensively in this process to ensure the
instructions are adequate and accurate. For the remainder of the study, patients will not be
able to take antibiotics, and fibre supplements. After the 3-week-long high FODMAP diet
period, participants will meet again with the dietician to obtain instructions on how to
consume a low FODMAP diet. After 3 weeks on a low FODMAP diet, all baseline testing will be
performed a fourth time. We aim to enroll 20 patients. Based on a 70% response rate to low
FODMAP diet (Halmos et al. 2014), and our experience in previous studies, this number should
be adequate.
Please note that the biopsies taken at sigmoidoscopy will be processed at HDH for the
supernatants, and then frozen for later electrophysiological studies at the Gastro-Intestinal
Diseases Research Unit (GIDRU) at KGH.
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