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通过对杂交鼠黏膜相关肠道微生物组的高分辨率遗传图谱分析揭示宿主-微生物相互作用的遗传结构和进化的关键特征。

Key features of the genetic architecture and evolution of host-microbe interactions revealed by high-resolution genetic mapping of the mucosa-associated gut microbiome in hybrid mice.

机构信息

Max Planck Institute for Evolutionary Biology, Plön, Germany.

Section of Evolutionary Medicine, Institute for Experimental Medicine, Kiel University, Kiel, Germany.

出版信息

Elife. 2022 Jul 19;11:e75419. doi: 10.7554/eLife.75419.

Abstract

Determining the forces that shape diversity in host-associated bacterial communities is critical to understanding the evolution and maintenance of metaorganisms. To gain deeper understanding of the role of host genetics in shaping gut microbial traits, we employed a powerful genetic mapping approach using inbred lines derived from the hybrid zone of two incipient house mouse species. Furthermore, we uniquely performed our analysis on microbial traits measured at the gut mucosal interface, which is in more direct contact with host cells and the immune system. Several mucosa-associated bacterial taxa have high heritability estimates, and interestingly, 16S rRNA transcript-based heritability estimates are positively correlated with cospeciation rate estimates. Genome-wide association mapping identifies 428 loci influencing 120 taxa, with narrow genomic intervals pinpointing promising candidate genes and pathways. Importantly, we identified an enrichment of candidate genes associated with several human diseases, including inflammatory bowel disease, and functional categories including innate immunity and G-protein-coupled receptors. These results highlight key features of the genetic architecture of mammalian host-microbe interactions and how they diverge as new species form.

摘要

确定塑造宿主相关细菌群落多样性的力量对于理解后生生物的进化和维持至关重要。为了更深入地了解宿主遗传学在塑造肠道微生物特征中的作用,我们利用了一种强大的遗传作图方法,该方法使用了源自两个初生家鼠物种杂交区的近交系。此外,我们还独特地对在肠道黏膜界面测量的微生物特征进行了分析,该界面与宿主细胞和免疫系统有更直接的接触。一些黏膜相关细菌类群具有较高的遗传力估计值,有趣的是,基于 16S rRNA 转录本的遗传力估计值与共进化率估计值呈正相关。全基因组关联作图确定了影响 120 个分类群的 428 个基因座,狭窄的基因组区间精确定位了有希望的候选基因和途径。重要的是,我们鉴定出了与多种人类疾病相关的候选基因的富集,包括炎症性肠病,以及包括先天免疫和 G 蛋白偶联受体在内的功能类别。这些结果突出了哺乳动物宿主-微生物相互作用的遗传结构的关键特征,以及随着新物种的形成它们如何发生分歧。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0bba/9307277/adea98d52dc1/elife-75419-fig1.jpg

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