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鉴定一种新型微菌素,可杀灭肠出血性大肠杆菌 O157:H7 和 O26。

Characterization of a novel microcin that kills enterohemorrhagic Escherichia coli O157:H7 and O26.

机构信息

Department of Veterinary Microbiology and Pathology, Washington State University, Pullman, Washington, USA.

出版信息

Appl Environ Microbiol. 2012 Sep;78(18):6592-9. doi: 10.1128/AEM.01067-12. Epub 2012 Jul 6.

Abstract

A novel phenotype was recently identified in which specific strains of Escherichia coli inhibit competing E. coli strains via a mechanism that was designated "proximity-dependent inhibition" (PDI). PDI-expressing (PDI(+)) E. coli is known to inhibit susceptible (PDI(-)) E. coli strains, including several enterohemorrhagic (EHEC) and enterotoxigenic (ETEC) E. coli strains. In this study, every strain from a genetically diverse panel of E. coli O157:H7 (n = 25) and additional strains of E. coli serovar O26 were susceptible to the PDI phenotype. LIVE/DEAD staining was consistent with inhibition by killing of susceptible cells. Comparative genome analysis identified the genetic component of PDI, which is composed of a plasmid-borne (Incl1) operon encoding a putative microcin and associated genes for transport, immunity, and microcin activation. Transfer of the plasmid to a PDI(-) strain resulted in transfer of the phenotype, and deletion of the genes within the operon resulted in loss of the inhibition phenotype. Deletion of chromosomally encoded tolC also resulted in loss of the inhibitory phenotype, and this confirmed that the putative microcin is most likely secreted via a type I secretion pathway. Deletion of an unrelated plasmid gene did not affect the PDI phenotype. Quantitative reverse transcription (RT)-PCR demonstrated that microcin expression is correlated with logarithmic-phase growth. The ability to inhibit a diversity of E. coli strains indicates that this microcin may influence gut community composition and could be useful for control of important enteric pathogens.

摘要

最近发现了一种新的表型,即特定的大肠杆菌菌株通过一种被称为“邻近依赖性抑制”(PDI)的机制抑制竞争的大肠杆菌菌株。已知表达 PDI(PDI(+))的大肠杆菌会抑制易感(PDI(-))的大肠杆菌菌株,包括几种肠出血性(EHEC)和肠毒性(ETEC)大肠杆菌菌株。在这项研究中,来自遗传多样化的大肠杆菌 O157:H7 (n = 25)和其他大肠杆菌血清型 O26 菌株的每一个菌株都对 PDI 表型敏感。LIVE/DEAD 染色与抑制敏感细胞的杀伤一致。比较基因组分析确定了 PDI 的遗传成分,它由质粒携带的(Incl1)操纵子组成,编码一种假定的微菌素和相关的运输、免疫和微菌素激活基因。将质粒转移到 PDI(-) 菌株中会导致表型转移,而删除操纵子内的基因会导致抑制表型丧失。删除染色体编码的 tolC 也会导致抑制表型丧失,这证实了假定的微菌素很可能通过 I 型分泌途径分泌。删除无关的质粒基因不会影响 PDI 表型。定量逆转录(RT)-PCR 表明微菌素的表达与对数期生长相关。抑制多种大肠杆菌菌株的能力表明,这种微菌素可能会影响肠道群落组成,并可用于控制重要的肠道病原体。

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