Gut microbiota signatures in inflammatory bowel disease

Author:

Vestergaard Marie Vibeke1ORCID,Allin Kristine H.12ORCID,Eriksen Carsten13ORCID,Zakerska‐Banaszak Oliwia4,Arasaradnam Ramesh P.5ORCID,Alam Mohammad T.56,Kristiansen Karsten17,Brix Susanne13,Jess Tine12

Affiliation:

1. Center for Molecular Prediction of Inflammatory Bowel Disease PREDICT Department of Clinical Medicine Aalborg University Copenhagen Denmark

2. Department of Gastroenterology & Hepatology Aalborg University Hospital Aalborg Denmark

3. Department of Biotechnology and Biomedicine Technical University of Denmark Lyngby Denmark

4. Institute of Human Genetics Polish Academy of Sciences Poznan Poland

5. Warwick Medical School & Cancer Research Centre University of Leicester Leicester UK

6. Department of Biology United Arab Emirates University Al Ain Abu Dhabi United Arab Emirates

7. Laboratory of Genomics and Molecular Medicine Department of Biology University of Copenhagen Copenhagen Denmark

Abstract

AbstractBackgroundInflammatory bowel diseases (IBD), including Crohn's disease (CD) and ulcerative colitis (UC), affect millions of people worldwide with increasing incidence.ObjectivesSeveral studies have shown a link between gut microbiota composition and IBD, but results are often limited by small sample sizes. We aimed to re‐analyze publicly available fecal microbiota data from IBD patients.MethodsWe extracted original fecal 16S rRNA amplicon sequencing data from 45 cohorts of IBD patients and healthy individuals using the BioProject database at the National Center for Biotechnology Information. Unlike previous meta‐analyses, we merged all study cohorts into a single dataset, including sex, age, geography, and disease information, based on which microbiota signatures were analyzed, while accounting for varying technical platforms.ResultsAmong 2518 individuals in the combined dataset, we discovered a hitherto unseen number of genera associated with IBD. A total of 77 genera associated with CD, of which 38 were novel associations, and a total of 64 genera associated with UC, of which 28 represented novel associations. Signatures were robust across different technical platforms and geographic locations. Reduced alpha diversity in IBD compared to healthy individuals, in CD compared to UC, and altered microbiota composition (beta diversity) in UC and especially in CD as compared to healthy individuals were found.ConclusionsCombining original microbiota data from 45 cohorts, we identified a hitherto unseen large number of genera associated with IBD. Identification of microbiota features robustly associated with CD and UC may pave the way for the identification of new treatment targets.

Funder

Danmarks Grundforskningsfond

Publisher

Wiley

Subject

Gastroenterology,Oncology

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