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大肠杆菌序列型131中膜内流和外流的调节对秀丽隐杆线虫模型中的细菌运动性、生物膜形成及毒力产生影响。

Modulation of Membrane Influx and Efflux in Escherichia coli Sequence Type 131 Has an Impact on Bacterial Motility, Biofilm Formation, and Virulence in a Caenorhabditis elegans Model.

作者信息

Pantel Alix, Dunyach-Remy Catherine, Ngba Essebe Christelle, Mesureur Jennifer, Sotto Albert, Pagès Jean-Marie, Nicolas-Chanoine Marie-Hélène, Lavigne Jean-Philippe

机构信息

Institut National de la Santé et de la Recherche Médicale, U1047, Université de Montpellier, UFR de Médecine, Nîmes, France Service de Microbiologie, CHU Carémeau, Nîmes University Hospital, Nîmes, France.

Institut National de la Santé et de la Recherche Médicale, U1047, Université de Montpellier, UFR de Médecine, Nîmes, France.

出版信息

Antimicrob Agents Chemother. 2016 Apr 22;60(5):2901-11. doi: 10.1128/AAC.02872-15. Print 2016 May.

Abstract

Energy-dependent efflux overexpression and altered outer membrane permeability (influx) can promote multidrug resistance (MDR). The present study clarifies the regulatory pathways that control membrane permeability in the pandemic clone Escherichia coli sequence type 131 (ST131) and evaluates the impact of efflux and influx modulations on biofilm formation, motility, and virulence in the Caenorhabditis elegans model. Mutants of two uropathogenic E. coli (UPEC) strains, MECB5 (ST131; H30-Rx) and CFT073 (ST73), as well as a fecal strain, S250 (ST131; H22), were in vitro selected using continuous subculture in subinhibitory concentrations of ertapenem (ETP), chloramphenicol (CMP), and cefoxitin (FOX). Mutations in genes known to control permeability were shown for the two UPEC strains: MECB5-FOX (deletion of 127 bp in marR; deletion of 1 bp and insertion of an IS1 element in acrR) and CFT073-CMP (a 1-bp deletion causing a premature stop in marR). We also demonstrated that efflux phenotypes in the mutants selected with CMP and FOX were related to the AcrAB-TolC pump, but also to other efflux systems. Alteration of membrane permeability, caused by underexpression of the two major porins, OmpF and OmpC, was shown in MECB5-ETP and mutants selected with FOX. Lastly, our findings suggest that efflux pump-overproducing isolates (CMP mutants) pose a serious threat in terms of virulence (significant reduction in worm median survival) and host colonization. Lack of porins (ETP and FOX mutants) led to a high level of antibiotic resistance in an H30-Rx subclone. Nevertheless, this adaptation created a physiological disadvantage (decreased motility and ability to form biofilm) associated with a low potential for virulence.

摘要

能量依赖型外排过表达和外膜通透性改变(内流)可促进多药耐药(MDR)。本研究阐明了控制大流行克隆大肠杆菌序列类型131(ST131)膜通透性的调控途径,并评估了外排和内流调节对秀丽隐杆线虫模型中生物膜形成、运动性和毒力的影响。使用亚抑菌浓度的厄他培南(ETP)、氯霉素(CMP)和头孢西丁(FOX)连续传代,在体外筛选了两种尿路致病性大肠杆菌(UPEC)菌株MECB5(ST131;H30-Rx)和CFT073(ST73)以及粪便菌株S250(ST131;H22)的突变体。在两种UPEC菌株中显示了已知控制通透性的基因突变:MECB5-FOX(marR中127 bp缺失;acrR中1 bp缺失并插入一个IS1元件)和CFT073-CMP(1 bp缺失导致marR中提前终止)。我们还证明,用CMP和FOX筛选出的突变体中的外排表型不仅与AcrAB-TolC泵有关,还与其他外排系统有关。在MECB5-ETP和用FOX筛选出的突变体中,显示出由两种主要孔蛋白OmpF和OmpC表达不足引起的膜通透性改变。最后,我们的研究结果表明,外排泵过度产生的分离株(CMP突变体)在毒力(蠕虫中位生存期显著缩短)和宿主定殖方面构成严重威胁。缺乏孔蛋白(ETP和FOX突变体)导致H30-Rx亚克隆中的高水平抗生素耐药性。然而,这种适应性产生了与低毒力潜力相关的生理劣势(运动性降低和形成生物膜的能力下降)。

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