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短尾stx噬菌体利用保守的YaeT蛋白在肠道细菌中传播志贺毒素基因。

Short-tailed stx phages exploit the conserved YaeT protein to disseminate Shiga toxin genes among enterobacteria.

作者信息

Smith Darren L, James Chloë E, Sergeant Martin J, Yaxian Yan, Saunders Jon R, McCarthy Alan J, Allison Heather E

机构信息

Microbiology Research Group, BioSciences Building, School of Biological Sciences, University of Liverpool, Crown Street, Liverpool, Merseyside, UK.

出版信息

J Bacteriol. 2007 Oct;189(20):7223-33. doi: 10.1128/JB.00824-07. Epub 2007 Aug 10.

Abstract

Infection of Escherichia coli by Shiga toxin-encoding bacteriophages (Stx phages) was the pivotal event in the evolution of the deadly Shiga toxin-encoding E. coli (STEC), of which serotype O157:H7 is the most notorious. The number of different bacterial species and strains reported to produce Shiga toxin is now more than 500, since the first reported STEC infection outbreak in 1982. Clearly, Stx phages are spreading rapidly, but the underlying mechanism for this dissemination has not been explained. Here we show that an essential and highly conserved gene product, YaeT, which has an essential role in the insertion of proteins in the gram-negative bacterial outer membrane, is the surface molecule recognized by the majority (ca. 70%) of Stx phages via conserved tail spike proteins associated with a short-tailed morphology. The yaeT gene was initially identified through complementation, and its role was confirmed in phage binding assays with and without anti-YaeT antiserum. Heterologous cloning of E. coli yaeT to enable Stx phage adsorption to Erwinia carotovora and the phage adsorption patterns of bacterial species possessing natural yaeT variants further supported this conclusion. The use of an essential and highly conserved protein by the majority of Stx phages is a strategy that has enabled and promoted the rapid spread of shigatoxigenic potential throughout multiple E. coli serogroups and related bacterial species. Infection of commensal bacteria in the mammalian gut has been shown to amplify Shiga toxin production in vivo, and the data from this study provide a platform for the development of a therapeutic strategy to limit this YaeT-mediated infection of the commensal flora.

摘要

携带志贺毒素的噬菌体(Stx噬菌体)感染大肠杆菌是致命的产志贺毒素大肠杆菌(STEC)进化过程中的关键事件,其中血清型O157:H7最为臭名昭著。自1982年首次报道STEC感染疫情以来,现已报道有超过500种不同的细菌物种和菌株可产生志贺毒素。显然,Stx噬菌体正在迅速传播,但其传播的潜在机制尚未得到解释。在此,我们表明一种必需且高度保守的基因产物YaeT在革兰氏阴性菌外膜蛋白插入过程中起关键作用,它是大多数(约70%)Stx噬菌体通过与短尾形态相关的保守尾刺蛋白识别的表面分子。yaeT基因最初通过互补作用得以鉴定,其作用在有无抗YaeT抗血清的噬菌体结合试验中得到证实。将大肠杆菌yaeT进行异源克隆以使Stx噬菌体能够吸附到胡萝卜软腐欧文氏菌上,以及具有天然yaeT变体的细菌物种的噬菌体吸附模式进一步支持了这一结论。大多数Stx噬菌体利用一种必需且高度保守的蛋白质,这是一种策略,使得产志贺毒素的潜力能够在多个大肠杆菌血清群和相关细菌物种中得以实现并促进其快速传播。已证明哺乳动物肠道中共生菌的感染会在体内放大志贺毒素的产生,本研究的数据为开发一种治疗策略提供了一个平台,以限制这种由YaeT介导的共生菌群感染。

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