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首页> 外文期刊>Antimicrobial agents and chemotherapy. >Variation in Resistance Traits, Phylogenetic Backgrounds, and Virulence Genotypes among Escherichia coli Clinical Isolates from Adjacent Hospital Campuses Serving Distinct Patient Populations
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Variation in Resistance Traits, Phylogenetic Backgrounds, and Virulence Genotypes among Escherichia coli Clinical Isolates from Adjacent Hospital Campuses Serving Distinct Patient Populations

机译:来自不同患者群体的相邻医院校园内大肠杆菌临床分离株的耐药性状,系统发育背景和毒力基因型的变化

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摘要

Escherichia coli sequence type 13 (ST131), an emergent cause of multidrug-resistant extraintestinal infections, has important phylogenetic subsets, notably the H30 and H30Rx subclones, with distinctive resistance profiles and, possibly, clinical associations. To clarify the local prevalence of these ST131 subclones and their associations with antimicrobial resistance, ecological source, and virulence traits, we extensively characterized 233 consecutive E. coli clinical isolates (July and August 2013) from the University of Minnesota Medical Center-Fairview Infectious Diseases and Diagnostic Laboratory, Minneapolis, MN, which serves three adjacent facilities (a children's hospital and low-and high-acuity adult facilities). ST131 accounted for 26% of the study isolates (more than any other clonal group), was distributed similarly by facility, and was closely associated with ciprofloxacin resistance and extended-spectrum beta-lactamase (ESBL) production. The H30 and H30Rx subclones accounted for most ST131 isolates and for the association of ST131 with fluoroquinolone resistance and ESBL production. Unlike ST131 per se, these subclones were distributed differentially by hospital, being most prevalent at the high-acuity adult facility and were absent from the children's hospital. The virulence gene profiles of ST131 and its subclones were distinctive and more extensive than those of other fluoroquinolone-resistant or ESBL-producing isolates. Within ST131, blaCTX-M-15 was confined to H30Rx isolates and other blaCTX-M variants to non-Rx H30 isolates. Pulsed-field gel electrophoresis documented a predominance of globally distributed pulsotypes and no local outbreak pattern. These findings help clarify the epidemiology, ecology, and bacterial correlates of the H30 and H30Rx ST131 subclones by documenting a high overall prevalence but significant segregation by facility, strong associations with fluoroquinolone resistance and specific ESBL variants, and distinctive virulence gene associations that may confer fitness advantages over other resistant E. coli.
机译:大肠杆菌13型序列(ST131)是多药耐药性肠外感染的紧急原因,具有重要的系统发生亚型,尤其是H30和H30Rx亚克隆,具有独特的耐药性以及可能的临床关联性。为了弄清这些ST131亚克隆在当地的流行情况以及它们与抗菌素耐药性,生态来源和毒力特性的关系,我们广泛地鉴定了明尼苏达大学医学中心-Fairview传染病连续233份大肠杆菌临床分离株(2013年7月和2013年8月)以及明尼苏达州明尼阿波利斯市的诊断实验室,为三个相邻的设施(儿童医院和低,高视力成人设施)提供服务。 ST131占研究菌株的26%(比其他任何克隆组都多),按设施分布相似,并且与环丙沙星耐药性和广谱β-内酰胺酶(ESBL)产生密切相关。 H30和H30Rx亚克隆占大多数ST131分离株,并与ST131与氟喹诺酮耐药性和ESBL产生有关。与ST131本身不同,这些亚克隆是按医院差异分布的,在高敏成人设施中最为普遍,而儿童医院则不在。 ST131及其亚克隆的毒力基因谱与其他对氟喹诺酮耐药或产生ESBL的菌株相比,具有独特性和广泛性。在ST131中,blaCTX-M-15仅限于H30Rx分离株,其他blaCTX-M变体仅限于非Rx H30分离株。脉冲场凝胶电泳记录了主要分布在全球的脉冲型,没有局部暴发模式。这些发现通过记录较高的总体患病率但按设施显着隔离,与氟喹诺酮耐药性和特定ESBL变体的强关联以及可能赋予适应性的独特毒力基因关联来帮助阐明H30和H30Rx ST131亚克隆的流行病学,生态学和细菌相关性优于其他抗性大肠杆菌。

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