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产 VIM-1 型肺炎克雷伯菌多位点序列型 15 医院感染暴发:分子基础、临床危险因素和结局。

Nosocomial outbreak of VIM-1-producing Klebsiella pneumoniae isolates of multilocus sequence type 15: molecular basis, clinical risk factors, and outcome.

机构信息

Servicio de Microbiología, Hospital Universitario Puerta de Hierro Majadahonda, Madrid, Spain.

出版信息

Antimicrob Agents Chemother. 2012 Jan;56(1):420-7. doi: 10.1128/AAC.05036-11. Epub 2011 Oct 17.

DOI:10.1128/AAC.05036-11
PMID:22005997
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3256054/
Abstract

We study the epidemiology, molecular basis, clinical risk factors, and outcome involved in the clonal dissemination of VIM-1-producing Klebsiella pneumoniae isolates in the hospital setting. All patients infected/colonized by carbapenem-nonsusceptible K. pneumoniae (CNSKP) in 2009 were included. Molecular epidemiology was studied by pulsed-field gel electrophoresis (PFGE) and multilocus sequence typing (MLST). Antibiotic resistance genes were analyzed by PCR and sequencing. Plasmids were studied by PFGE with S1 nuclease digestion and for incompatibility group by a PCR-based replicon typing scheme. Risk factors associated with CNSKP colonization/infection were assessed by an observational case-control study. All 55 patients studied were infected (n = 28) or colonized (n = 27) by VIM-1-producing K. pneumoniae. All but one acquired isolates of a single clone (PFGE cluster 1 [C1], sequence type 15 [ST15]), while another clone (PFGE C2, ST340) was detected in four patients. C1 isolates also produced the new extended-spectrum β-lactamase SHV-134. bla(VIM-1) was carried in a class 1 integron and an untypeable plasmid of ∼50 bp. The number of days that the patient received mechanical ventilation, the use of parenteral nutrition, previous treatment with linezolid, and treatment with extended-spectrum cephalosporins for more than 7 days were detected to be independent risk factors for CNSKP acquisition. The VIM-1-producing K. pneumoniae ST15 clone has a high capacity to spread among intensive care unit patients with severe underlying conditions. A high rate of associated mortality and great difficulty in controlling the spread of this clone, without permanent behavioral changes in the personnel, were observed.

摘要

我们研究了产 VIM-1 肺炎克雷伯菌在医院环境中克隆传播的流行病学、分子基础、临床危险因素和结局。所有 2009 年感染/定植碳青霉烯类药物不敏感肺炎克雷伯菌(CNSKP)的患者均纳入研究。采用脉冲场凝胶电泳(PFGE)和多位点序列分型(MLST)进行分子流行病学研究。采用 PCR 和测序分析抗生素耐药基因。通过 PFGE 结合 S1 核酸酶消化和基于 PCR 的复制子分型方案研究质粒。通过观察性病例对照研究评估与 CNSKP 定植/感染相关的危险因素。研究的 55 名患者均感染(n = 28)或定植(n = 27)产 VIM-1 肺炎克雷伯菌。除 1 例患者外,所有患者均获得单一克隆(PFGE 簇 1 [C1],序列型 15 [ST15])的分离株,另有 1 例患者(PFGE C2,ST340)在 4 例患者中检测到。C1 分离株还产生新的扩展谱β-内酰胺酶 SHV-134。bla(VIM-1)位于 1 类整合子和一个约 50 bp 的未定型质粒中。患者接受机械通气的天数、接受肠外营养、先前使用利奈唑胺治疗以及使用超广谱头孢菌素治疗超过 7 天被检测为 CNSKP 获得的独立危险因素。产 VIM-1 肺炎克雷伯菌 ST15 克隆具有在重症监护病房重症患者中广泛传播的高能力。观察到高死亡率、控制该克隆传播的巨大困难以及在人员中没有永久性行为改变。

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