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阿尔及利亚社区获得性尿路致病性大肠杆菌的抗生素耐药性、毒力及遗传背景

Antibiotic Resistance, Virulence, and Genetic Background of Community-Acquired Uropathogenic Escherichia coli from Algeria.

作者信息

Yahiaoui Merzouk, Robin Frédéric, Bakour Rabah, Hamidi Moufida, Bonnet Richard, Messai Yamina

机构信息

1 Laboratory of Cellular and Molecular Biology, Faculty of Biological Sciences, University of Sciences and Technology Houari Boumediene , Algiers, Algeria .

2 CHU Clermont-Ferrand, Laboratoire de Bactériologie , Clermont-Ferrand, France .

出版信息

Microb Drug Resist. 2015 Oct;21(5):516-26. doi: 10.1089/mdr.2015.0045. Epub 2015 Jun 1.

Abstract

The aim of the study was to investigate antibiotic resistance mechanisms, virulence traits, and genetic background of 150 nonrepetitive community-acquired uropathogenic Escherichia coli (CA-UPEC) from Algeria. A rate of 46.7% of isolates was multidrug resistant. bla genes detected were blaTEM (96.8% of amoxicillin-resistant isolates), blaCTX-M-15 (4%), overexpressed blaAmpC (4%), blaSHV-2a, blaTEM-4, blaTEM-31, and blaTEM-35 (0.7%). All tetracycline-resistant isolates (51.3%) had tetA and/or tetB genes. Sulfonamides and trimethoprim resistance genes were sul2 (60.8%), sul1 (45.9%), sul3 (6.7%), dfrA14 (25.4%), dfrA1 (18.2%), dfrA12 (16.3%), and dfrA25 (5.4%). High-level fluoroquinolone resistance (22.7%) was mediated by mutations in gyrA (S83L-D87N) and parC (S80I-E84G/V or S80I) genes. qnrB5, qnrS1, and aac(6')-Ib-cr were rare (5.3%). Class 1 and/or class 2 integrons were detected (40.7%). Isolates belonged to phylogroups B2+D (50%), A+B1 (36%), and F+C+Clade I (13%). Most of D (72.2%) and 38.6% of B2 isolates were multidrug resistant; they belong to 14 different sequence types, including international successful ST131, ST73, and ST69, reported for the first time in the community in Algeria and new ST4494 and ST4529 described in this study. Besides multidrug resistance, B2 and D isolates possessed virulence factors of colonization, invasion, and long-term persistence. The study highlighted multidrug-resistant CA-UPEC with high virulence traits and an epidemic genetic background.

摘要

本研究的目的是调查来自阿尔及利亚的150株非重复性社区获得性尿路致病性大肠杆菌(CA-UPEC)的抗生素耐药机制、毒力特征和遗传背景。46.7%的分离株对多种药物耐药。检测到的bla基因有blaTEM(对阿莫西林耐药的分离株中占96.8%)、blaCTX-M-15(4%)、过表达的blaAmpC(4%)、blaSHV-2a、blaTEM-4、blaTEM-31和blaTEM-35(0.7%)。所有四环素耐药分离株(51.3%)都有tetA和/或tetB基因。磺胺类和甲氧苄啶耐药基因有sul2(60.8%)、sul1(45.9%)、sul3(6.7%)、dfrA14(25.4%)、dfrA1(18.2%)、dfrA12(16.3%)和dfrA25(5.4%)。高水平氟喹诺酮耐药(22.7%)由gyrA(S83L-D87N)和parC(S80I-E84G/V或S80I)基因的突变介导。qnrB5、qnrS1和aac(6')-Ib-cr很少见(5.3%)。检测到1类和/或2类整合子(40.7%)。分离株属于B2+D菌系群(50%)、A+B1菌系群(36%)和F+C+进化枝I菌系群(13%)。大多数D菌系群(72.2%)和38.6%的B2分离株对多种药物耐药;它们属于14种不同的序列类型,包括国际上流行的ST131、ST73和ST69,这是在阿尔及利亚社区首次报道,以及本研究中描述的新序列类型ST4494和ST4529。除了对多种药物耐药外,B2和D分离株还具有定植、侵袭和长期存活的毒力因子。该研究突出了具有高毒力特征和流行遗传背景的多重耐药CA-UPEC。

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