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序列分析和特征描述可转移的混合质粒,其编码多药耐药性,并使肠外大肠杆菌具有人畜共患的潜力。

Sequence analysis and characterization of a transferable hybrid plasmid encoding multidrug resistance and enabling zoonotic potential for extraintestinal Escherichia coli.

机构信息

Department of Veterinary and Biomedical Sciences, University of Minnesota, Saint Paul, Minnesota 55108, USA.

出版信息

Infect Immun. 2010 May;78(5):1931-42. doi: 10.1128/IAI.01174-09. Epub 2010 Feb 16.

Abstract

ColV plasmids of extraintestinal pathogenic Escherichia coli (ExPEC) encode a variety of fitness and virulence factors and have long been associated with septicemia and avian colibacillosis. These plasmids are found significantly more often in ExPEC, including ExPEC associated with human neonatal meningitis and avian colibacillosis, than in commensal E. coli. Here we describe pAPEC-O103-ColBM, a hybrid RepFIIA/FIB plasmid harboring components of the ColV pathogenicity island and a multidrug resistance (MDR)-encoding island. This plasmid is mobilizable and confers the ability to cause septicemia in chickens, the ability to cause bacteremia resulting in meningitis in the rat model of human disease, and the ability to resist the killing effects of multiple antimicrobial agents and human serum. The results of a sequence analysis of this and other ColV plasmids supported previous findings which indicated that these plasmid types arose from a RepFIIA/FIB plasmid backbone on multiple occasions. Comparisons of pAPEC-O103-ColBM with other sequenced ColV and ColBM plasmids indicated that there is a core repertoire of virulence genes that might contribute to the ability of some ExPEC strains to cause high-level bacteremia and meningitis in a rat model. Examination of a neonatal meningitis E. coli (NMEC) population revealed that approximately 58% of the isolates examined harbored ColV-type plasmids and that 26% of these plasmids had genetic contents similar to that of pAPEC-O103-ColBM. The linkage of the ability to confer MDR and the ability contribute to multiple forms of human and animal disease on a single plasmid presents further challenges for preventing and treating ExPEC infections.

摘要

肠外致病性大肠杆菌(ExPEC)的 ColV 质粒编码多种适应性和毒力因子,长期以来一直与败血症和禽大肠杆菌病有关。这些质粒在 ExPEC 中更为常见,包括与人类新生儿脑膜炎和禽大肠杆菌病相关的 ExPEC,而在共生大肠杆菌中则不常见。在这里,我们描述了 pAPEC-O103-ColBM,这是一种携带 ColV 致病性岛和多药耐药(MDR)编码岛成分的混合 RepFIIA/FIB 质粒。该质粒可移动,并赋予鸡引起败血症的能力、在人类疾病大鼠模型中引起菌血症导致脑膜炎的能力以及抵抗多种抗菌药物和人血清杀伤作用的能力。对该质粒和其他 ColV 质粒进行序列分析的结果支持了先前的发现,即这些质粒类型多次从 RepFIIA/FIB 质粒骨架中产生。将 pAPEC-O103-ColBM 与其他已测序的 ColV 和 ColBM 质粒进行比较表明,存在一组核心毒力基因,可能有助于某些 ExPEC 菌株在大鼠模型中引起高水平菌血症和脑膜炎的能力。对新生儿脑膜炎大肠杆菌(NMEC)群体的检查表明,约 58%的被检查分离株携带 ColV 型质粒,其中 26%的质粒具有与 pAPEC-O103-ColBM 相似的遗传内容。将赋予 MDR 的能力和导致人类和动物多种疾病的能力与单个质粒联系起来,给预防和治疗 ExPEC 感染带来了进一步的挑战。

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