对临床分离的含有巨型质粒的拉菲诺斯肠球菌 Er676 和 ATCC49464 的封闭基因组组装进行种间多样性和功能基因组分析。

Access Microbiology Pub Date : 2023-06-12 eCollection Date: 2023-01-01 DOI:10.1099/acmi.0.000508.v3
Belle M Sharon, Neha V Hulyalkar, Philippe E Zimmern, Kelli L Palmer, Nicole J De Nisco
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引用次数: 0

摘要

拉菲诺斯肠球菌(Enterococcus raffinosus)是一种未被充分研究的肠球菌属成员,其特有的巨型质粒导致基因组体积庞大。虽然与其他肠球菌相比,该菌与人类感染相关的情况较少,但它能致病,并能在肠道、尿道、血液和环境等不同环境中存活。迄今为止,很少有关于 E. raffinosus 的完整基因组组装发表。在这项研究中,我们报告了第一个临床尿路拉菲诺斯大肠杆菌菌株 Er676 的完整组装结果,该菌株是从一名绝经后、有反复尿路感染病史的妇女体内分离出来的。我们还完成了临床型菌株 ATCC49464 的组装。基因组比较分析显示了大型附属基因组驱动的种间多样性。一个保守的巨型质粒的存在表明,它是拉菲诺斯大肠杆菌无处不在的重要遗传特征。我们发现 E. raffinosus 染色体富含 DNA 复制和蛋白质生物合成基因,而巨型质粒富含转录和碳水化合物代谢基因。噬菌体分析表明,染色体和巨质体序列的多样性部分来自水平基因转移。Er676 的基因组大小是迄今为止报告的 E. raffinosus 最大的,对人类致病的可能性也是最高的。Er676 还拥有多个抗菌药耐药性基因,其中除一个基因外,其他基因都在染色体上编码,而且拥有最完整的噬菌体序列。通过对 Er676 和 ATCC49464 基因组的完整组装和比较分析,可以深入了解 E. raffinosus 的种间多样性,这种多样性赋予了它在人体内定殖和存活的能力。研究导致该物种致病性的遗传因素将为防治这种机会性病原体引起的疾病提供宝贵的工具。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Inter-species diversity and functional genomic analyses of closed genome assemblies of clinically isolated, megaplasmid-containing <i>Enterococcus raffinosus</i> Er676 and ATCC49464.

Inter-species diversity and functional genomic analyses of closed genome assemblies of clinically isolated, megaplasmid-containing <i>Enterococcus raffinosus</i> Er676 and ATCC49464.

Inter-species diversity and functional genomic analyses of closed genome assemblies of clinically isolated, megaplasmid-containing <i>Enterococcus raffinosus</i> Er676 and ATCC49464.

Inter-species diversity and functional genomic analyses of closed genome assemblies of clinically isolated, megaplasmid-containing Enterococcus raffinosus Er676 and ATCC49464.

Enterococcus raffinosus is an understudied member of its genus possessing a characteristic megaplasmid contributing to a large genome size. Although less commonly associated with human infection compared to other enterococci, this species can cause disease and persist in diverse niches such as the gut, urinary tract, blood and environment. Few complete genome assemblies have been published to date for E. raffinosus . In this study, we report the complete assembly of the first clinical urinary E. raffinosus strain, Er676, isolated from a postmenopausal woman with history of recurrent urinary tract infection. We additionally completed the assembly of clinical type strain ATCC49464. Comparative genomic analyses reveal inter-species diversity driven by large accessory genomes. The presence of a conserved megaplasmid indicates it is a ubiquitous and vital genetic feature of E. raffinosus . We find that the E. raffinosus chromosome is enriched for DNA replication and protein biosynthesis genes while the megaplasmid is enriched for transcription and carbohydrate metabolism genes. Prophage analysis suggests that diversity in the chromosome and megaplasmid sequences arises, in part, from horizontal gene transfer. Er676 demonstrated the largest genome size reported to date for E. raffinosus and the highest probability of human pathogenicity. Er676 also possesses multiple antimicrobial resistance genes, of which all but one are encoded on the chromosome, and has the most complete prophage sequences. Complete assembly and comparative analyses of the Er676 and ATCC49464 genomes provide important insight into the inter-species diversity of E. raffinosus that gives it its ability to colonize and persist in the human body. Investigating genetic factors that contribute to the pathogenicity of this species will provide valuable tools to combat diseases caused by this opportunistic pathogen.

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