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来自爱尔兰都柏林的产头孢他啶酶大肠杆菌临床分离株耐药性的分子流行病学研究

The Molecular Epidemiology of Resistance in Cefotaximase-Producing Escherichia coli Clinical Isolates from Dublin, Ireland.

作者信息

Burke Liam, Humphreys Hilary, Fitzgerald-Hughes Deirdre

机构信息

1 Department of Clinical Microbiology, Royal College of Surgeons in Ireland, Beaumont Hospital , Dublin 9, Ireland .

2 Department of Microbiology, Beaumont Hospital , Dublin 9, Ireland .

出版信息

Microb Drug Resist. 2016 Oct;22(7):552-558. doi: 10.1089/mdr.2015.0154. Epub 2016 Mar 22.

Abstract

In view of continued high clinical prevalence of infections involving extended-spectrum β-lactamase (ESBL)-producing Escherichia coli, this study sought to characterise the blaCTX-M genes, their associated mobile genetic elements and the integrons present in 100 ESBL-producing E. coli isolates collected in a Dublin hospital and associated community healthcare facilities. Polymerase chain reaction (PCR) mapping and sequencing was used to detect blaCTX-M alleles, their associated insertion sequences (ISs) and class 1 and 2 integrons in the collection. ESBL plasmids were characterised by PCR-based replicon typing and replicon sequence typing (RST). Cefotaximases were harboured by 94% of isolates (66 blaCTX-M-15, 8 blaCTX-M-14, 7 blaCTX-M-1, 4 blaCTX-M-3, 3 blaCTX-M-9, 2 blaCTX-M-27, 2 blaCTX-M-55, 1 blaCTX-M-32 and 1 blaCTX-M-2). An ISEcp1 promoter was linked to a group 1 blaCTX-M gene in 45% of isolates. A further 34% of isolates contained blaCTX-M-15 downstream of IS26, an arrangement typical of epidemic UK strain A. Class 1 integrons were found in 66% of isolates, most carrying trimethoprim/aminoglycoside resistance genes. CTX-M plasmids were primarily of multireplicon IncF or IncI1 type, but IncN and unidentified types were also found. Novel IncF RSTs F1:A-:B-, F45:A1:B-, F45:A4:B- and a novel IncI1 sequence type, ST159, were identified. CTX-M plasmids and integrons resembled those identified recently in animal isolates from Ireland and Western Europe. The molecular epidemiology of CTX-M-producing E. coli in Dublin suggests that horizontal spread of mobile genetic elements contributes to antimicrobial resistant human infections. Further investigations into whether animals or animal products represent an important local reservoir for these elements are warranted.

摘要

鉴于产超广谱β-内酰胺酶(ESBL)的大肠埃希菌感染在临床上持续高发,本研究旨在对都柏林一家医院及相关社区医疗设施收集的100株产ESBL大肠埃希菌分离株中的blaCTX-M基因、其相关的移动遗传元件及整合子进行特征分析。采用聚合酶链反应(PCR)图谱分析和测序来检测收集菌株中的blaCTX-M等位基因、其相关的插入序列(IS)以及1类和2类整合子。通过基于PCR的复制子分型和复制子序列分型(RST)对ESBL质粒进行特征分析。94%的分离株携带头孢噻肟酶(66株携带blaCTX-M-15、8株携带blaCTX-M-14、7株携带blaCTX-M-1、4株携带blaCTX-M-3、3株携带blaCTX-M-9、2株携带blaCTX-M-27、2株携带blaCTX-M-55、1株携带blaCTX-M-32和1株携带blaCTX-M-2)。45%的分离株中,ISEcp1启动子与1组blaCTX-M基因相连。另外34%的分离株在IS26下游含有blaCTX-M-15,这是英国流行菌株A的典型排列方式。66%的分离株中发现了1类整合子,大多数携带甲氧苄啶/氨基糖苷类耐药基因。CTX-M质粒主要为多复制子IncF或IncI1型,但也发现了IncN型和未鉴定类型。鉴定出了新型IncF RSTs F1:A-:B-、F45:A1:B-、F45:A4:B-以及一种新型IncI1序列类型ST159。CTX-M质粒和整合子与最近在爱尔兰和西欧动物分离株中鉴定出的相似。都柏林产CTX-M大肠埃希菌的分子流行病学表明,移动遗传元件的水平传播导致了人类抗菌药物耐药感染。有必要进一步调查动物或动物产品是否是这些元件的重要本地储存库。

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