Comparative Metagenomics Revealed Commonly Enriched Gene Sets in Human Gut Microbiomes

Ken Kurokawa(Nara Institute of Science and Technology), Takehiko Itoh(Mitsubishi Research Institute (Japan)), Tomomi Kuwahara(Tokushima University), Kenshiro Oshima(Kitasato University), Hidehiro Toh(Kitasato Institute Hospital), Atsushi Toyoda(RIKEN Center for Integrative Medical Sciences), Hideto Takami(Japan Agency for Marine-Earth Science and Technology), Hidetoshi Morita(Azabu University), Vineet K. Sharma(RIKEN Center for Integrative Medical Sciences), T Srivastava(RIKEN Center for Integrative Medical Sciences), Todd D. Taylor(RIKEN Center for Integrative Medical Sciences), Hideki Noguchi(The University of Tokyo), Hiroshi Mori(Nara Institute of Science and Technology), Yoshitoshi Ogura(University of Miyazaki), Dusko S. Ehrlich(Département Génétique Animale), Kikuji Itoh(The University of Tokyo), Toshihisa Takagi(The University of Tokyo), Yoshiyuki Sakaki(RIKEN Center for Integrative Medical Sciences), Tetsuya Hayashi(University of Miyazaki), Masahira Hattori(RIKEN Center for Integrative Medical Sciences)
DNA Research
January 1, 2007
Cited by 855Open Access
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Abstract

Numerous microbes inhabit the human intestine, many of which are uncharacterized or uncultivable. They form a complex microbial community that deeply affects human physiology. To identify the genomic features common to all human gut microbiomes as well as those variable among them, we performed a large-scale comparative metagenomic analysis of fecal samples from 13 healthy individuals of various ages, including unweaned infants. We found that, while the gut microbiota from unweaned infants were simple and showed a high inter-individual variation in taxonomic and gene composition, those from adults and weaned children were more complex but showed a high functional uniformity regardless of age or sex. In searching for the genes over-represented in gut microbiomes, we identified 237 gene families commonly enriched in adult-type and 136 families in infant-type microbiomes, with a small overlap. An analysis of their predicted functions revealed various strategies employed by each type of microbiota to adapt to its intestinal environment, suggesting that these gene sets encode the core functions of adult and infant-type gut microbiota. By analysing the orphan genes, 647 new gene families were identified to be exclusively present in human intestinal microbiomes. In addition, we discovered a conjugative transposon family explosively amplified in human gut microbiomes, which strongly suggests that the intestine is a 'hot spot' for horizontal gene transfer between microbes.


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