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物种-功能关系塑造了人类肠道微生物组的生态特性。

Species-function relationships shape ecological properties of the human gut microbiome.

机构信息

Department of Microbiology and Immunology, KU Leuven-University of Leuven, Rega Institute, Herestraat 49, B-3000 Leuven, Belgium.

VIB, Center for the Biology of Disease, Herestraat 49, B-3000 Leuven, Belgium.

出版信息

Nat Microbiol. 2016 Jun 13;1(8):16088. doi: 10.1038/nmicrobiol.2016.88.

Abstract

Despite recent progress, the organization and ecological properties of the intestinal microbial ecosystem remain under-investigated. Here, using a manually curated metabolic module framework for (meta-)genomic data analysis, we studied species-function relationships in gut microbial genomes and microbiomes. Half of gut-associated species were found to be generalists regarding overall substrate preference, but we observed significant genus-level metabolic diversification linked to bacterial life strategies. Within each genus, metabolic consistency varied significantly, being low in Firmicutes genera and higher in Bacteroides. Differentiation of fermentable substrate degradation potential contributed to metagenomic functional repertoire variation between individuals, with different enterotypes showing distinct saccharolytic/proteolytic/lipolytic profiles. Finally, we found that module-derived functional redundancy was reduced in the low-richness Bacteroides enterotype, potentially indicating a decreased resilience to perturbation, in line with its frequent association to dysbiosis. These results provide insights into the complex structure of gut microbiome-encoded metabolic properties and emphasize the importance of functional and ecological assessment of gut microbiome variation in clinical studies.

摘要

尽管最近取得了进展,但肠道微生物生态系统的组织和生态特性仍未得到充分研究。在这里,我们使用手动 curated 的代谢模块框架来进行(宏)基因组数据分析,研究了肠道微生物基因组和微生物组中的物种-功能关系。发现一半的肠道相关物种在总体底物偏好方面是通才,但我们观察到与细菌生活策略相关的显著属水平代谢多样化。在每个属内,代谢一致性差异很大,在厚壁菌门属中较低,而在拟杆菌门属中较高。可发酵底物降解潜力的分化导致个体间宏基因组功能谱的变化,不同的肠型表现出不同的发酵/蛋白水解/脂肪水解特征。最后,我们发现,在低丰度拟杆菌肠型中,模块衍生的功能冗余减少,这可能表明其对扰动的恢复能力降低,与它与失调的频繁关联一致。这些结果提供了对肠道微生物组编码代谢特性复杂结构的深入了解,并强调了在临床研究中对肠道微生物组变异进行功能和生态评估的重要性。

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