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首页> 外文期刊>Pathogens and disease[electronic] >Proteomic response of beta-lactamases-producing Enterobacter cloacae complex strain to cefotaxime-induced stress
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Proteomic response of beta-lactamases-producing Enterobacter cloacae complex strain to cefotaxime-induced stress

机译:蛋白质组学的反应beta-lactamases-producing肠杆菌属泄殖腔复杂应变cefotaxime-induced压力

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摘要

Bacteria of the Enterobacter cloacae complex are among the ten most common pathogens causing nosocomial infections in the USA. Consequently, increased resistance to beta-lactam antibiotics, particularly expanded-spectrum cephalosporins like cefotaxime (CTX), poses a serious threat. Differential In-Gel Electrophoresis (DIGE), followed by LC-MS/MS analysis and bioinformatics tools, was employed to investigate the survival mechanisms of a multidrug-resistant E. hormaechei subsp. steigerwaltii 51 carrying several beta-lactamase-encoding genes, including the 'pandemic' bla(CTX-M-15). After exposing the strain with sub-minimal inhibitory concentration (MIC) of CTX, a total of 1072 spots from the whole-cell proteome were detected, out of which 35 were differentially expressed (P = 1.5). Almost 50% of these proteins were involved in cell metabolism and energy production, and then cell wall organization/virulence, stress response and transport. This is the first study investigating the whole-cell proteomic response related to the survival of beta-lactamases-producing strain, belonging to the E. cloacae complex when exposed to beta-lactam antibiotic. Our data support the theory of a multifactorial synergistic effect of diverse proteomic changes occurring in bacterial cells during antibiotic exposure, depicting the complexity of beta-lactam resistance and giving us an insight in the key pathways mediating the antibiotic resistance in this emerging opportunistic pathogen.
机译:肠杆菌属的细菌泄殖腔复杂在十大最常见的病原体引起在美国医院感染。增加抗beta-lactam抗生素,尤其是expanded-spectrum头孢菌素如头孢噻肟(CTX),构成了严重的威胁。微分为胶液电泳(消化),其次是质/ MS分析和生物信息学工具,是用来调查生存耐多药大肠hormaechei的机制无性系种群。beta-lactamase-encoding基因,包括“流行”bla (CTX-M-15)。应变与sub-minimal抑制浓度CTX (MIC),共1072点全细胞蛋白质组发现的35是差异表达(P = 1.5)。参与细胞代谢和能量生产,然后细胞壁组织/毒性反应和压力交通工具。全细胞蛋白质组的反应有关beta-lactamases-producing的生存压力,属于大肠泄殖腔复杂当暴露beta-lactam抗生素。理论的多因子的协同效应不同的蛋白质组变化发生在细菌细胞在抗生素暴露,描绘了的复杂性beta-lactam阻力和给予我们关键通路介导的洞察力在这个新兴的抗生素耐药性投机取巧的病原体。

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