A17 SYSTEMS-LEVEL PATHWAY MAPPING REVEALS GUT–BRAIN AND IMMUNE SIGNATURES IN FLARES OF IBS
V Mohan, M Pinto-Sanchez, A Nardelli, M Magee, R Borojevic, Z Kroezen, M Shanmuganathan, G De Palma, P Moayyedi, P Britz Mckibbin, S Collins, P Bercik

TL;DR
This study maps gut-microbiota and immune pathways in IBS flare-ups, revealing individualized signatures that could improve precision treatment.
Contribution
The study introduces microbiota-metabolite-gene-signaling pathway networks to uncover individualized IBS flare mechanisms.
Findings
Neuroactive ligand–receptor interaction was the most frequently altered pathway in IBS flares.
Pathway incidence clustering showed mechanistic heterogeneity independent of clinical IBS subtypes.
Immune-related pathways like NET formation were prominent in some IBS-D subjects.
Abstract
Irritable bowel syndrome (IBS) is a disorder of gut-brain interaction affecting an estimated 5.8% of Canadians (Rome IV criteria). Although accumulating evidence implicates the gut microbiota in IBS pathophysiology, identifying the key drivers of symptom expression remains challenging due to pronounced interindividual variability. We hypothesized that individualized microbiota–metabolite interactions may drive distinct host pathway responses underlying symptom variability during flares. To identify signaling pathways underlying flare-associated microbiota–metabolite signatures in IBS patients. Subjects with microbiota (16S rRNA sequencing) and metabolite (untargeted metabolomics) alterations linked to symptom flares were identified from a 25-week longitudinal cohort of 28 IBS patients (∼950 samples). For each subject, altered metabolites were integrated with microbial associations and…
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Taxonomy
TopicsGastrointestinal motility and disorders · Gut microbiota and health · Inflammatory Bowel Disease
