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首页> 外文期刊>The Journal of Infectious Diseases >Genome-wide Screening Identifies Phosphotransferase System Permease BepA to Be Involved in Enterococcus faecium Endocarditis and Biofilm Formation
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Genome-wide Screening Identifies Phosphotransferase System Permease BepA to Be Involved in Enterococcus faecium Endocarditis and Biofilm Formation

机译:基因组筛选鉴定磷酸裂解酶系统允许释放酶涉及肠球菌粪便心内膜炎和生物膜形成

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摘要

Enterococcus faecium is a common cause of nosocomial infections, of which infective endocarditis is associated with substantial mortality. In this study, we used a microarray-based transposon mapping (M-TraM) approach to evaluate a rat endocarditis model and identified a gene, originally annotated as "fruA" and renamed "bepA," putatively encoding a carbohydrate phosphotransferase system (PTS) permease (biofilm and endocarditis-associated permease A [BepA]), as important in infective endocarditis. This gene is highly enriched in E. faecium clinical isolates and absent in commensal isolates that are not associated with infection. Confirmation of the phenotype was established in a competition experiment of wild-type and a markerless bepA mutant in a rat endocarditis model. In addition, deletion of bepA impaired biofilm formation in vitro in the presence of 100% human serum and metabolism of beta-methyl-D-glucoside. beta-glucoside metabolism has been linked to the metabolism of glycosaminoglycans that are exposed on injured heart valves, where bacteria attach and form vegetations. Therefore, we propose that the PTS permease BepA is directly implicated in E. faecium pathogenesis.
机译:肠球菌粪便是医院感染的常见原因,其中感染性心内膜炎与大量死亡率有关。在这项研究中,我们使用了一种基于微阵列的转座子映射(M-Tram)方法来评估大鼠心内膜炎模型,并确定最初被注释为“FRUA”并更名为“BEPA”的基因,借助于碳水化合物磷酸转移酶系统(PTS)允许(生物膜和心内膜炎相关允许[BEPA]),在感染性心内膜炎中重要。该基因高度富含E.粪便临床分离物,并且不存在与感染无关的共生分离物。在大鼠心内膜炎模型中的野生型和无明显BEPA突变体的竞争试验中建立了表型。此外,在100%人血清的存在下,在体外缺失Bepa受损的生物膜形成和β-甲基-D-葡糖苷的代谢。 β-葡萄糖苷代谢已与暴露在受伤的心脏瓣膜暴露的糖胺聚糖的代谢有关,其中细菌附着和形成植被。因此,我们提出PTS允许BEPA直接涉及E.粪便发病机制。

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