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一种新型的 IS26 结构环绕着来自德国临床大肠杆菌分离株的不同质粒中的 blaCTX-M 基因。

A novel IS26 structure surrounds blaCTX-M genes in different plasmids from German clinical Escherichia coli isolates.

机构信息

Robert Koch Institute, Burgstraße 37, 38855 Wernigerode, Germany.

Institute of Medical Microbiology and Hygiene, University Hospital of Ulm, Steinhövelstraße 9, 89075 Ulm, Germany.

出版信息

J Med Microbiol. 2010 May;59(Pt 5):580-587. doi: 10.1099/jmm.0.016188-0. Epub 2010 Jan 21.

DOI:10.1099/jmm.0.016188-0
PMID:20093380
Abstract

This report focuses on the molecular characterization of 22 extended-spectrum beta-lactamase-producing Escherichia coli isolates collected in a German university hospital during a period of 9 months in 2006. Relationship analysis of clinical isolates was done via PFGE, multilocus sequence typing, plasmid profiling and additionally PCR for bla(ESBL) detection and determination of phylogroups. After conjugal transfer, plasmid isolation and subsequent PCR for bla(ESBL) detection and determination of incompatibility groups were performed. Using one-primer walking, up to 3600 bp upstream and downstream of different bla(CTX-M) genes could be sequenced. beta-Lactamases found were TEM-1 (n=14), SHV-5 (n=1) and a wide variety of CTX-M types (n=21), i.e. CTX-M-15 (n=12), CTX-M-1 (n=4), CTX-M-14 (n=2), CTX-M-9 (n=1), CTX-M-3 (n=1) and one new type, CTX-M-65 (n=1). In 18 isolates, bla(ESBL) genes were located on conjugative plasmids of sizes between 40 and 180 kbp belonging to incompatibility groups FII (n=9), N (n=5) and I1 (n=4). bla(CTX-M) was found to be associated with the common elements ISEcp1, IS26 and IS903-D, but with unusual spacer sequences for ISEcp1 in two isolates. These insertion sequences, connected to bla(CTX-M) as well as other genes, were located between two IS26 elements in a configuration that has not yet been described. The results reveal the emergence of bla(ESBL), predominantly bla(CTX-M), located on different plasmids harboured by genotypically different E. coli strains. The identical gene arrangement in the bla(CTX-M) neighbourhood in plasmids of different incompatibility groups indicates a main role of IS26 in distribution of mobile resistance elements between different plasmids.

摘要

本报告重点介绍了 2006 年 9 个月期间在德国一家大学医院收集的 22 株产超广谱β-内酰胺酶的大肠杆菌分离株的分子特征。通过 PFGE、多位点序列分型、质粒图谱分析以及 bla(ESBL)检测和确定菌株群的 PCR 对临床分离株进行关系分析。进行了接合转移、质粒分离以及随后的 bla(ESBL)检测和确定不相容群的 PCR 后,使用单引物行走,对不同 bla(CTX-M)基因上下游的 3600bp 进行了测序。发现的β-内酰胺酶为 TEM-1(n=14)、SHV-5(n=1)和多种 CTX-M 型(n=21),即 CTX-M-15(n=12)、CTX-M-1(n=4)、CTX-M-14(n=2)、CTX-M-9(n=1)、CTX-M-3(n=1)和一种新型 CTX-M-65(n=1)。在 18 株分离株中,bla(ESBL)基因位于大小在 40 至 180kbp 之间的可接合质粒上,属于不相容群 FII(n=9)、N(n=5)和 I1(n=4)。发现 bla(CTX-M)与常见元件 ISEcp1、IS26 和 IS903-D 相关,但在两个分离株中 ISEcp1 的间隔序列不寻常。这些插入序列与 bla(CTX-M)以及其他基因相连,位于两个 IS26 元件之间,这种配置尚未被描述。结果显示,bla(ESBL),主要是 bla(CTX-M),位于不同质粒上,这些质粒由基因型不同的大肠杆菌菌株携带。不同不相容群质粒中 bla(CTX-M)周围基因排列相同,表明 IS26 在不同质粒之间移动耐药元件的分布中起主要作用。

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