Disease-specific loss of microbial cross-feeding interactions in the human gut

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作者
Vanessa R. Marcelino
Caitlin Welsh
Christian Diener
Emily L. Gulliver
Emily L. Rutten
Remy B. Young
Edward M. Giles
Sean M. Gibbons
Chris Greening
Samuel C. Forster
机构
[1] Monash University,Department of Molecular and Translational Sciences
[2] Hudson Institute of Medical Research,Centre for Innate Immunity and Infectious Diseases
[3] University of Melbourne,Melbourne Integrative Genomics, School of BioSciences
[4] University of Melbourne,Department of Microbiology and Immunology at the Peter Doherty Institute for Infection and Immunity
[5] Biomedicine Discovery Institute,Department of Microbiology
[6] Institute for Systems Biology,Department of Paediatrics
[7] Monash University,Department of Bioengineering
[8] University of Washington,Department of Genome Sciences
[9] University of Washington,eScience Institute
[10] University of Washington,undefined
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Many gut microorganisms critical to human health rely on nutrients produced by each other for survival; however, these cross-feeding interactions are still challenging to quantify and remain poorly characterized. Here, we introduce a Metabolite Exchange Score (MES) to quantify those interactions. Using metabolic models of prokaryotic metagenome-assembled genomes from over 1600 individuals, MES allows us to identify and rank metabolic interactions that are significantly affected by a loss of cross-feeding partners in 10 out of 11 diseases. When applied to a Crohn’s disease case-control study, our approach identifies a lack of species with the ability to consume hydrogen sulfide as the main distinguishing microbiome feature of disease. We propose that our conceptual framework will help prioritize in-depth analyses, experiments and clinical targets, and that targeting the restoration of microbial cross-feeding interactions is a promising mechanism-informed strategy to reconstruct a healthy gut ecosystem.
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