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. 2021 Feb;53(2):147-155.
doi: 10.1038/s41588-020-00747-1. Epub 2021 Jan 18.

Genome-wide association study in 8,956 German individuals identifies influence of ABO histo-blood groups on gut microbiome

Malte Christoph Rühlemann  1 Britt Marie Hermes  2   3   4 Corinna Bang  1 Shauni Doms  2   3 Lucas Moitinho-Silva  1   5 Louise Bruun Thingholm  1 Fabian Frost  6 Frauke Degenhardt  1 Michael Wittig  1 Jan Kässens  1 Frank Ulrich Weiss  6 Annette Peters  7   8 Klaus Neuhaus  9 Uwe Völker  10 Henry Völzke  10 Georg Homuth  10 Stefan Weiss  6   10 Harald Grallert  7 Matthias Laudes  11 Wolfgang Lieb  12 Dirk Haller  9   13 Markus M Lerch  6 John F Baines  2   3 Andre Franke  14
Affiliations

Genome-wide association study in 8,956 German individuals identifies influence of ABO histo-blood groups on gut microbiome

Malte Christoph Rühlemann et al. Nat Genet. 2021 Feb.

Abstract

The intestinal microbiome is implicated as an important modulating factor in multiple inflammatory1,2, neurologic3 and neoplastic diseases4. Recent genome-wide association studies yielded inconsistent, underpowered and rarely replicated results such that the role of human host genetics as a contributing factor to microbiome assembly and structure remains uncertain5-11. Nevertheless, twin studies clearly suggest host genetics as a driver of microbiome composition11. In a genome-wide association analysis of 8,956 German individuals, we identified 38 genetic loci to be associated with single bacteria and overall microbiome composition. Further analyses confirm the identified associations of ABO histo-blood groups and FUT2 secretor status with Bacteroides and Faecalibacterium spp. Mendelian randomization analysis suggests causative and protective effects of gut microbes, with clade-specific effects on inflammatory bowel disease. This holistic investigative approach of the host, its genetics and its associated microbial communities as a 'metaorganism' broaden our understanding of disease etiology, and emphasize the potential for implementing microbiota in disease treatment and management.

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References

    1. Lloyd-Price, J. et al. Multi-omics of the gut microbial ecosystem in inflammatory bowel diseases. Nature 569, 655–662 (2019). - PubMed - PMC - DOI
    1. Franzosa, E. A. et al. Gut microbiome structure and metabolic activity in inflammatory bowel disease. Nat. Microbiol. 4, 293–305 (2019). - PubMed - DOI
    1. Cryan, J. F., O’Riordan, K. J., Sandhu, K., Peterson, V. & Dinan, T. G. The gut microbiome in neurological disorders. Lancet Neurol. 19, 179–194 (2019). - PubMed - DOI
    1. Wirbel, J. et al. Meta-analysis of fecal metagenomes reveals global microbial signatures that are specific for colorectal cancer. Nat. Med. 25, 679–689 (2019). - PubMed - PMC - DOI
    1. Blekhman, R. et al. Host genetic variation impacts microbiome composition across human body sites. Genome Biol. 16, 191 (2015). - PubMed - PMC - DOI

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