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人类微生物组的宏基因组组装质粒在不同疾病队列中存在差异。

Metagenomic assembled plasmids of the human microbiome vary across disease cohorts.

机构信息

APC Microbiome Ireland, University College Cork, Co. Cork, Ireland.

School of Microbiology, University College Cork, Co. Cork, Ireland.

出版信息

Sci Rep. 2022 Jun 2;12(1):9212. doi: 10.1038/s41598-022-13313-y.

Abstract

We compiled a human metagenome assembled plasmid (MAP) database and interrogated differences across multiple studies that were originally designed to investigate the composition of the human microbiome across various lifestyles, life stages and events. This was performed as plasmids enable bacteria to rapidly expand their functional capacity through mobilisation, yet their contribution to human health and disease is poorly understood. We observed that inter-sample β-diversity differences of plasmid content (plasmidome) could distinguish cohorts across a multitude of conditions. We also show that reduced intra-sample plasmidome α-diversity is consistent amongst patients with inflammatory bowel disease (IBD) and Clostridioides difficile infections. We also show that faecal microbiota transplants can restore plasmidome diversity. Overall plasmidome diversity, specific plasmids, and plasmid-encoded functions can all potentially act as biomarkers of IBD or its severity. The human plasmidome is an overlooked facet of the microbiome and should be integrated into investigations regarding the role of the microbiome in promoting health or disease. Including MAP databases in analyses will enable a greater understanding of the roles of plasmid-encoded functions within the gut microbiome and will inform future human metagenome analyses.

摘要

我们编制了一个人类宏基因组组装质粒 (MAP) 数据库,并对多个最初旨在研究各种生活方式、生命阶段和事件下人类微生物组组成的研究进行了差异分析。这是因为质粒使细菌能够通过移动迅速扩大其功能能力,但它们对人类健康和疾病的贡献仍知之甚少。我们观察到质粒含量(质粒组)的样本间β多样性差异可以区分多种情况下的队列。我们还表明,炎症性肠病 (IBD) 和艰难梭菌感染患者的样本内质粒组 α多样性降低。我们还表明,粪便微生物群移植可以恢复质粒组多样性。总体而言,质粒组多样性、特定质粒和质粒编码的功能都可能作为 IBD 或其严重程度的生物标志物。人类质粒组是微生物组中被忽视的一个方面,应该将其纳入关于微生物组在促进健康或疾病方面的作用的研究中。在分析中包含 MAP 数据库将有助于更好地了解质粒编码功能在肠道微生物组中的作用,并为未来的人类宏基因组分析提供信息。

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