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在临床菌尿症期间,肠杆菌会分泌一种铜绿假单胞菌毒力抑制剂。

Enterobacteria secrete an inhibitor of Pseudomonas virulence during clinical bacteriuria.

作者信息

Ohlemacher Shannon I, Giblin Daryl E, d'Avignon D André, Stapleton Ann E, Trautner Barbara W, Henderson Jeffrey P

机构信息

Center for Women's Infectious Diseases Research.

Division of Infectious Diseases.

出版信息

J Clin Invest. 2017 Nov 1;127(11):4018-4030. doi: 10.1172/JCI92464. Epub 2017 Sep 25.

Abstract

Escherichia coli and other Enterobacteriaceae are among the most common pathogens of the human urinary tract. Among the genetic gains of function associated with urinary E. coli isolates is the Yersinia high pathogenicity island (HPI), which directs the biosynthesis of yersiniabactin (Ybt), a virulence-associated metallophore. Using a metabolomics approach, we found that E. coli and other Enterobacteriaceae expressing the Yersinia HPI also secrete escherichelin, a second metallophore whose chemical structure matches a known synthetic inhibitor of the virulence-associated pyochelin siderophore system in Pseudomonas aeruginosa. We detected escherichelin during clinical E. coli urinary tract infection (UTI) and experimental human colonization with a commensal, potentially probiotic E. coli bacteriuria strain. Escherichelin production by colonizing enterobacteria may help human hosts resist opportunistic infections by Pseudomonas and other pyochelin-expressing bacteria. This siderophore-based mechanism of microbial antagonism may be one of many elements contributing to the protective effects of the human microbiome. Future UTI-preventive probiotic strains may benefit by retaining the escherichelin biosynthetic capacity of the Yersinia HPI while eliminating the Ybt biosynthetic capacity.

摘要

大肠杆菌和其他肠杆菌科细菌是人类泌尿道最常见的病原体之一。与泌尿道大肠杆菌分离株相关的功能获得性基因中,有耶尔森菌高致病性岛(HPI),它指导yersiniabactin(Ybt)的生物合成,Ybt是一种与毒力相关的金属载体。通过代谢组学方法,我们发现表达耶尔森菌HPI的大肠杆菌和其他肠杆菌科细菌还分泌埃希菌素,这是另一种金属载体,其化学结构与铜绿假单胞菌中与毒力相关的绿脓菌素铁载体系统的已知合成抑制剂相匹配。我们在临床大肠杆菌尿路感染(UTI)以及用共生的、可能具有益生菌特性的大肠杆菌菌尿菌株进行的实验性人类定植过程中检测到了埃希菌素。定植的肠杆菌产生埃希菌素可能有助于人类宿主抵抗铜绿假单胞菌和其他表达绿脓菌素的细菌的机会性感染。这种基于铁载体的微生物拮抗机制可能是有助于人类微生物组发挥保护作用的众多因素之一。未来预防UTI的益生菌菌株可能会受益于保留耶尔森菌HPI的埃希菌素生物合成能力,同时消除Ybt生物合成能力。

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