Ulcerative Colitis Clinical Trial
Official title:
A Prospective Longitudinal Study of Fecal Microbiome and Calprotectin to Predict Relapse in Patients With Inflammatory Bowel Disease
Inflammatory bowel disease (IBD) is a chronic idiopathic inflammatory condition of the
intestine, which results in diarrhea, rectal bleeding, urgency, weight loss and abdominal
pain. The natural course of IBD is characterized by activity outbreaks and periods of
remission. In most cases, relapses in Crohn's disease (CD) and in ulcerative colitis (UC) are
unpredictable and despite effective medical treatment, a degree of subclinical inflammation
may persist in the bowel wall, contributing to a significant risk of relapse.
In IBD, altered fecal microbiota signatures have been consistently reported which included a
reduction in biodiversity with lower proportions of Firmicutes and increases in
Proteobacteria and Bacteroidetes phylum members.
It is however unclear whether changes in microbial profile including diversity and
composition can predict disease relapse in IBD. We hypothesize that fecal microbial
signatures in conjunction with fecal calprotectin may play a role in predicting relapse in
IBD patients.
Inflammatory bowel disease (IBD) is a chronic idiopathic inflammatory condition of the
intestine, which results in diarrhea, rectal bleeding, urgency, weight loss and abdominal
pain. The natural course of IBD is characterized by activity outbreaks and periods of
remission. In most cases, relapses in Crohn's disease (CD) and in ulcerative colitis (UC) are
unpredictable and despite effective medical treatment, a degree of subclinical inflammation
may persist in the bowel wall, contributing to a significant risk of relapse.
Endoscopy has been used to monitor a disease but it is time-consuming, costly, invasive, and
associated with certain risks of morbidity. Many patients are reluctant to undergo repeated
endoscopic examinations, particularly when their disease is quiescent. Acute phase reactants
have been used but their sensitivity and specificity in correlating to intestinal
inflammatory activity are very low, and their capacity to predict disease relapse is poor and
controversial. A number of fecal biomarkers have been evaluated for their utility for
monitoring and predicting relapse in IBD but some of these biomarkers are also not specific.
In IBD, altered fecal microbiota signatures have been consistently reported which included a
reduction in biodiversity with lower proportions of Firmicutes and increases in
Proteobacteria and Bacteroidetes phylum members. In addition, disease remission and relapse
are associated with microbial changes in both mucosal and fecal samples. In particular, a
loss of species richness in Crohn's disease has been widely observed. Recently microbial
biomarkers may differentiate between CD and UC. Furthermore, different microbial groups are
associated with smoking habit and localization of the disease in CD and UC. It is however
unclear whether changes in microbial profile including diversity and composition can predict
disease relapse in IBD. We hypothesize that fecal microbial signatures in conjunction with
fecal calprotectin may play a role in predicting relapse in IBD patients.
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