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Staphylococcus epidermidis clones express Staphylococcus aureus-type wall teichoic acid to shift from a commensal to pathogen lifestyle

表皮葡萄球菌 微生物学 地氯酸 生物 金黄色葡萄球菌 毒力 病菌 殖民地化 葡萄球菌感染 细菌 基因 遗传学
作者
Xin Du,Jesper Larsen,Min Li,Axel Walter,Christoph Slavetinsky,Anna Both,Patricia Sanchez‐Carballo,Marc Stegger,Esther Lehmann,Yao Liu,Junlan Liu,Jessica Slavetinsky,Katarzyna Duda,Bernhard Krismer,Simon Heilbronner,Christopher Weidenmaier,Christoph Mayer,Holger Rohde,Volker Winstel,Andreas Peschel
出处
期刊:Nature microbiology [Nature Portfolio]
卷期号:6 (6): 757-768 被引量:49
标识
DOI:10.1038/s41564-021-00913-z
摘要

Most clonal lineages of Staphylococcus epidermidis are commensals present on human skin and in the nose. However, some globally spreading healthcare-associated and methicillin-resistant S. epidermidis (HA-MRSE) clones are major causes of difficult-to-treat implant or bloodstream infections. The molecular determinants that alter the lifestyle of S. epidermidis have remained elusive, and their identification might provide therapeutic targets. We reasoned that changes in surface-exposed wall teichoic acid (WTA) polymers of S. epidermidis, which potentially shape host interactions, may be linked to differences between colonization and infection abilities of different clones. We used a combined epidemiological and functional approach to show that while commensal clones express poly-glycerolphosphate WTA, S. epidermidis multilocus sequence type 23, which emerged in the past 15 years and is one of the main infection-causing HA-MRSE clones, contains an accessory genetic element, tarIJLM, that leads to the production of a second, Staphylococcus aureus-type WTA (poly-ribitolphosphate (RboP)). Production of RboP-WTA by S. epidermidis impaired in vivo colonization but augmented endothelial attachment and host mortality in a mouse sepsis model. tarIJLM was absent from commensal human sequence types but was found in several other HA-MRSE clones. Moreover, RboP-WTA enabled S. epidermidis to exchange DNA with S. aureus via siphovirus bacteriophages, thereby creating a possible route for the inter-species exchange of methicillin resistance, virulence and colonization factors. We conclude that tarIJLM alters the lifestyle of S. epidermidis from commensal to pathogenic and propose that RboP-WTA might be a robust target for preventive and therapeutic interventions against MRSE infections. The presence of an accessory genetic element, tarIJLM—which leads to the production of a S. aureus-type wall teichoic acid—alters the lifestyle of S. epidermidis invasive clones, impairing in vivo mouse colonization but increasing endothelial attachment and host mortality.
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