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在美国300型菌株中,移动遗传元件在封闭的医院环境中逐渐丧失。

Gradual loss of mobile genetic elements in USA300 in a closed hospital niche.

作者信息

Ranc Anne-Gaelle, Simões Patricia Martins, Youenou Benjamin, Kolenda Camille, Dupieux Céline, Laurent Frédéric, Rasigade Jean Philippe, Tristan Anne, Vandenesch François

机构信息

Centre National de Référence des Staphylocoques, Institut des agents infectieux, Hospices Civils de Lyon, F-69004 Lyon, France.

CIRI, Center for Integrative Research in Infectious diseases and Immunology, Université de Lyon, Inserm U1111, Université Claude Bernard Lyon 1, CNRS UMR5308, ENS de Lyon, F-69007 Lyon, France.

出版信息

ISME Commun. 2025 Jun 26;5(1):ycaf105. doi: 10.1093/ismeco/ycaf105. eCollection 2025 Jan.

Abstract

Our French National Reference Centre for Staphylococci was requested to determine the epidemiological link between 19 methicillin-susceptible/resistant Staphylococcus aureus (MSSA/MRSA) isolates obtained from patients and a healthcare worker in a long-term care hospital, following the death of a nurse from pneumonia presumed to be associated with the drainage of a patient with an active skin infection. Whole genome sequencing was performed on all isolates to characterize their virulome, resistome, and phylogenetic relationships. Phylogenetic analysis revealed that 12 isolates belonged to the North American USA300 lineage, which is the predominant MRSA in North America but is less prevalent in Europe. USA300 strains are typically described as belonging to the clonal complex 8 (CC8) and possessing several mobile genetic elements (MGEs): the pathogenicity island SaPI5, the PVL-encoding bacteriophage ϕSa2USA, the staphylococcal chromosomal cassette IVa (SCCIVa), and the arginine catabolic mobile element (ACME). All 12 isolates lacked SaPI5, and four possessed the other typical MGEs of the USA300 lineage. However, one isolate did not carry SCCIVa, six did not have ACME, and two did not carry ϕSa2USA. The topology of the phylogenetic tree and the phylodynamic analysis suggested the loss of SaPI5 before entry in the long-term hospital, which may have occurred 3-4 years before the current outbreak. As long-term hospital may represent a relatively closed and stable ecosystem, we concluded that this loss of MGEs is a phenomenon of genetic diversification driven by niche specialization, in this case, originally constituted by a healthcare institution.

摘要

在一名护士因疑似与一名患有活动性皮肤感染患者的引流相关的肺炎死亡后,我们法国国家葡萄球菌参考中心被要求确定从一家长期护理医院的患者和一名医护人员身上分离出的19株甲氧西林敏感/耐药金黄色葡萄球菌(MSSA/MRSA)之间的流行病学联系。对所有分离株进行了全基因组测序,以表征它们的毒力组、耐药组和系统发育关系。系统发育分析表明,12株分离株属于北美USA300谱系,这是北美主要的MRSA,但在欧洲不太常见。USA300菌株通常被描述为属于克隆复合体8(CC8),并拥有几个移动遗传元件(MGEs):致病岛SaPI5、编码杀白细胞素的噬菌体ϕSa2USA、葡萄球菌染色体盒IVa(SCCIVa)和精氨酸分解代谢移动元件(ACME)。所有12株分离株均缺乏SaPI5,4株拥有USA300谱系的其他典型MGEs。然而,一株分离株未携带SCCIVa,6株没有ACME,2株未携带ϕSa2USA。系统发育树的拓扑结构和系统发育动力学分析表明,SaPI5在进入长期护理医院之前就已丢失,这可能发生在当前疫情爆发前3 - 4年。由于长期护理医院可能代表一个相对封闭和稳定的生态系统,我们得出结论,这种MGEs的丢失是一种由生态位特化驱动的遗传多样化现象,在这种情况下,最初是由一个医疗机构构成的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0fc6/12265888/c769925691ff/ycaf105f1.jpg

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