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Gut microbial co-abundance networks show specificity in inflammatory bowel disease and obesity

Author

Listed:
  • Lianmin Chen

    (University Medical Center Groningen
    University Medical Center Groningen)

  • Valerie Collij

    (University Medical Center Groningen
    University Medical Center Groningen)

  • Martin Jaeger

    (Radboud University Medical Center)

  • Inge C. L. van den Munckhof

    (Radboud University Medical Center)

  • Arnau Vich Vila

    (University Medical Center Groningen
    University Medical Center Groningen)

  • Alexander Kurilshikov

    (University Medical Center Groningen)

  • Ranko Gacesa

    (University Medical Center Groningen
    University Medical Center Groningen)

  • Trishla Sinha

    (University Medical Center Groningen)

  • Marije Oosting

    (Radboud University Medical Center)

  • Leo A. B. Joosten

    (Radboud University Medical Center
    Iuliu Hatieganu University of Medicine and Pharmacy)

  • Joost H. W. Rutten

    (Radboud University Medical Center)

  • Niels P. Riksen

    (Radboud University Medical Center)

  • Ramnik J. Xavier

    (Massachusetts General Hospital
    Broad Institute of MIT and Harvard
    Massachusetts General Hospital and Harvard Medical School
    Massachusetts Institute of Technology)

  • Folkert Kuipers

    (University Medical Center Groningen
    University Medical Center Groningen)

  • Cisca Wijmenga

    (University Medical Center Groningen
    University of Groningen)

  • Alexandra Zhernakova

    (University Medical Center Groningen)

  • Mihai G. Netea

    (Radboud University Medical Center
    University of Bonn
    Craiova University of Medicine and Pharmacy)

  • Rinse K. Weersma

    (University Medical Center Groningen)

  • Jingyuan Fu

    (University Medical Center Groningen
    University Medical Center Groningen)

Abstract

The gut microbiome is an ecosystem that involves complex interactions. Currently, our knowledge about the role of the gut microbiome in health and disease relies mainly on differential microbial abundance, and little is known about the role of microbial interactions in the context of human disease. Here, we construct and compare microbial co-abundance networks using 2,379 metagenomes from four human cohorts: an inflammatory bowel disease (IBD) cohort, an obese cohort and two population-based cohorts. We find that the strengths of 38.6% of species co-abundances and 64.3% of pathway co-abundances vary significantly between cohorts, with 113 species and 1,050 pathway co-abundances showing IBD-specific effects and 281 pathway co-abundances showing obesity-specific effects. We can also replicate these IBD microbial co-abundances in longitudinal data from the IBD cohort of the integrative human microbiome (iHMP-IBD) project. Our study identifies several key species and pathways in IBD and obesity and provides evidence that altered microbial abundances in disease can influence their co-abundance relationship, which expands our current knowledge regarding microbial dysbiosis in disease.

Suggested Citation

  • Lianmin Chen & Valerie Collij & Martin Jaeger & Inge C. L. van den Munckhof & Arnau Vich Vila & Alexander Kurilshikov & Ranko Gacesa & Trishla Sinha & Marije Oosting & Leo A. B. Joosten & Joost H. W. , 2020. "Gut microbial co-abundance networks show specificity in inflammatory bowel disease and obesity," Nature Communications, Nature, vol. 11(1), pages 1-12, December.
  • Handle: RePEc:nat:natcom:v:11:y:2020:i:1:d:10.1038_s41467-020-17840-y
    DOI: 10.1038/s41467-020-17840-y
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