Kurokawa Ken, Itoh Takehiko, Kuwahara Tomomi, Oshima Kenshiro, Toh Hidehiro, Toyoda Atsushi, Takami Hideto, Morita Hidetoshi, Sharma Vineet K, Srivastava Tulika P, Taylor Todd D, Noguchi Hideki, Mori Hiroshi, Ogura Yoshitoshi, Ehrlich Dusko S, Itoh Kikuji, Takagi Toshihisa, Sakaki Yoshiyuki, Hayashi Tetsuya, Hattori Masahira
Laboratory of Comparative Genomics, Graduate School of Information Science, Nara Institute of Science and Technology, Ikoma, Nara, Japan.
DNA Res. 2007 Aug 31;14(4):169-81. doi: 10.1093/dnares/dsm018. Epub 2007 Oct 3.
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.
众多微生物栖息于人类肠道,其中许多尚未得到充分表征或无法培养。它们形成了一个复杂的微生物群落,对人类生理机能有着深远影响。为了确定所有人类肠道微生物群落共有的基因组特征以及其中的可变特征,我们对包括未断奶婴儿在内的13名不同年龄健康个体的粪便样本进行了大规模比较宏基因组分析。我们发现,未断奶婴儿的肠道微生物群较为简单,在分类和基因组成上个体间差异很大,而成年人和断奶儿童的肠道微生物群则更为复杂,但无论年龄或性别,其功能具有高度一致性。在寻找肠道微生物群落中过度表达的基因时,我们确定了237个在成人型微生物群落中普遍富集的基因家族和136个在婴儿型微生物群落中富集的基因家族,两者重叠较少。对其预测功能的分析揭示了每种类型的微生物群适应肠道环境所采用的各种策略,这表明这些基因集编码了成人型和婴儿型肠道微生物群的核心功能。通过分析孤儿基因,我们确定了647个仅存在于人类肠道微生物群落中的新基因家族。此外,我们发现了一个在人类肠道微生物群落中爆发式扩增的接合转座子家族,这强烈表明肠道是微生物间水平基因转移的“热点”。
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