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大规模筛选靶向粪肠球菌突变文库鉴定包膜适应因子。

Large-scale screening of a targeted Enterococcus faecalis mutant library identifies envelope fitness factors.

机构信息

INRA, UMR1319 Micalis, Jouy-en-Josas, France.

出版信息

PLoS One. 2011;6(12):e29023. doi: 10.1371/journal.pone.0029023. Epub 2011 Dec 15.

Abstract

Spread of antibiotic resistance among bacteria responsible for nosocomial and community-acquired infections urges for novel therapeutic or prophylactic targets and for innovative pathogen-specific antibacterial compounds. Major challenges are posed by opportunistic pathogens belonging to the low GC% gram-positive bacteria. Among those, Enterococcus faecalis is a leading cause of hospital-acquired infections associated with life-threatening issues and increased hospital costs. To better understand the molecular properties of enterococci that may be required for virulence, and that may explain the emergence of these bacteria in nosocomial infections, we performed the first large-scale functional analysis of E. faecalis V583, the first vancomycin-resistant isolate from a human bloodstream infection. E. faecalis V583 is within the high-risk clonal complex 2 group, which comprises mostly isolates derived from hospital infections worldwide. We conducted broad-range screenings of candidate genes likely involved in host adaptation (e.g., colonization and/or virulence). For this purpose, a library was constructed of targeted insertion mutations in 177 genes encoding putative surface or stress-response factors. Individual mutants were subsequently tested for their i) resistance to oxidative stress, ii) antibiotic resistance, iii) resistance to opsonophagocytosis, iv) adherence to the human colon carcinoma Caco-2 epithelial cells and v) virulence in a surrogate insect model. Our results identified a number of factors that are involved in the interaction between enterococci and their host environments. Their predicted functions highlight the importance of cell envelope glycopolymers in E. faecalis host adaptation. This study provides a valuable genetic database for understanding the steps leading E. faecalis to opportunistic virulence.

摘要

耐抗生素细菌在医院获得性和社区获得性感染中的传播促使人们寻找新的治疗或预防靶点以及创新的针对病原体的抗菌化合物。低 GC%革兰氏阳性菌中的机会性病原体带来了主要挑战。其中,粪肠球菌是导致与危及生命的问题和增加医院成本相关的医院获得性感染的主要原因。为了更好地了解可能与毒力相关的肠球菌的分子特性,并解释这些细菌在医院感染中的出现,我们对来自人类血流感染的第一个万古霉素耐药分离株 V583 进行了首次大规模的粪肠球菌功能分析。V583 属于高风险克隆复合体 2 组,该组主要包含来自全球医院感染的分离株。我们对可能参与宿主适应(如定植和/或毒力)的候选基因进行了广泛筛选。为此,构建了一个包含 177 个编码假定表面或应激反应因子的基因靶向插入突变的文库。随后,逐个测试了突变体的以下特性:i)对氧化应激的抗性,ii)抗生素抗性,iii)对调理吞噬作用的抗性,iv)对人结肠癌细胞系 Caco-2 的黏附性,v)在替代昆虫模型中的毒力。我们的结果确定了一些参与肠球菌与其宿主环境相互作用的因素。它们的预测功能突出了细胞包膜糖聚合物在粪肠球菌宿主适应中的重要性。这项研究为理解导致粪肠球菌成为机会性病原体的毒力的步骤提供了有价值的遗传数据库。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3663/3240637/5decdb904849/pone.0029023.g001.jpg

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