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一个新的克隆群体彻底席卷:大肠杆菌序列类型131的神秘出现。

A new clone sweeps clean: the enigmatic emergence of Escherichia coli sequence type 131.

作者信息

Banerjee Ritu, Johnson James R

机构信息

Department of Pediatric and Adolescent Medicine, Mayo Clinic, Rochester, Minnesota, USA

Veterans Affairs Medical Center and University of Minnesota, Minneapolis, Minnesota, USA.

出版信息

Antimicrob Agents Chemother. 2014 Sep;58(9):4997-5004. doi: 10.1128/AAC.02824-14. Epub 2014 May 27.

Abstract

Escherichia coli sequence type 131 (ST131) is an extensively antimicrobial-resistant E. coli clonal group that has spread explosively throughout the world. Recent molecular epidemiologic and whole-genome phylogenetic studies have elucidated the fine clonal structure of ST131, which comprises multiple ST131 subclones with distinctive resistance profiles, including the (nested) H30, H30-R, and H30-Rx subclones. The most prevalent ST131 subclone, H30, arose from a single common fluoroquinolone (FQ)-susceptible ancestor containing allele 30 of fimH (type 1 fimbrial adhesin gene). An early H30 subclone member acquired FQ resistance and launched the rapid expansion of the resulting FQ-resistant subclone, H30-R. Subsequently, a member of H30-R acquired the CTX-M-15 extended-spectrum beta-lactamase and launched the rapid expansion of the CTX-M-15-containing subclone within H30-R, H30-Rx. Clonal expansion clearly is now the dominant mechanism for the rising prevalence of both FQ resistance and CTX-M-15 production in ST131 and in E. coli generally. Reasons for the successful dissemination and expansion of the key ST131 subclones remain undefined but may include increased transmissibility, greater ability to colonize and/or persist in the intestine or urinary tract, enhanced virulence, and more-extensive antimicrobial resistance compared to other E. coli. Here we discuss the epidemiology and molecular phylogeny of ST131 and its key subclones, possible mechanisms for their ecological success, implications of their widespread dissemination, and future research needs.

摘要

大肠杆菌序列类型131(ST131)是一个具有广泛抗菌耐药性的大肠杆菌克隆群,已在全球范围内迅速传播。最近的分子流行病学和全基因组系统发育研究阐明了ST131的精细克隆结构,它由多个具有独特耐药谱的ST131亚克隆组成,包括(嵌套的)H30、H30-R和H30-Rx亚克隆。最常见的ST131亚克隆H30起源于一个单一的常见氟喹诺酮(FQ)敏感祖先,该祖先含有fimH(1型菌毛粘附素基因)的等位基因30。H30亚克隆的一个早期成员获得了FQ耐药性,并促使由此产生的FQ耐药亚克隆H30-R迅速扩张。随后,H30-R的一个成员获得了CTX-M-15超广谱β-内酰胺酶,并促使H30-R内含有CTX-M-15的亚克隆H30-Rx迅速扩张。克隆扩张显然是目前ST131以及一般大肠杆菌中FQ耐药性和CTX-M-15产生率上升的主要机制。关键ST131亚克隆成功传播和扩张的原因尚不清楚,但可能包括与其他大肠杆菌相比,传播能力增强、在肠道或泌尿道定植和/或持续存在的能力更强、毒力增强以及抗菌耐药性更广泛。在此,我们讨论ST131及其关键亚克隆的流行病学和分子系统发育、它们在生态上成功的可能机制、它们广泛传播的影响以及未来的研究需求。

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