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天然免疫在促进金黄色葡萄球菌中SaeR/S介导的毒力方面的作用。

The role of innate immunity in promoting SaeR/S-mediated virulence in Staphylococcus aureus.

作者信息

Zurek Oliwia W, Nygaard Tyler K, Watkins Robert L, Pallister Kyler B, Torres Victor J, Horswill Alexander R, Voyich Jovanka M

机构信息

Department of Immunology and Infectious Diseases, Montana State University, Bozeman, Mont., USA.

出版信息

J Innate Immun. 2014;6(1):21-30. doi: 10.1159/000351200. Epub 2013 Jun 29.

Abstract

The ability of Staphylococcus aureus to infect tissues is dependent on precise control of virulence through gene-regulatory systems. While the SaeR/S two-component system has been shown to be a major regulator of S. aureus virulence, the influence of the host environment on SaeR/S-regulated genes (saeR/S targets) remains incompletely defined. Using QuantiGene 2.0 transcriptional assays, we examined expression of genes with the SaeR binding site in USA300 exposed to human and mouse neutrophils and host-derived peptides and during subcutaneous skin infection. We found that only some of the saeR/S targets, as opposed to the entire SaeR/S virulon, were activated within 5 and 10 min of interacting with human neutrophils as well as α-defensin. Furthermore, mouse neutrophils promoted transcription of saeR/S targets despite lacking α-defensin, and the murine skin environment elicited a distinctive expression profile of saeR/S targets. These findings indicate that saeR/S-mediated transcription is unique to and dependent on specific host stimuli. By using isogenic USA300ΔsaeR/S and USA300Δagr knockout strains, we also determined that SaeR/S is the major regulator of virulence factors, while Agr, a quorum-sensing two-component system, has moderate influence on transcription of the saeR/S targets under the tested physiological conditions.

摘要

金黄色葡萄球菌感染组织的能力取决于通过基因调控系统对毒力的精确控制。虽然SaeR/S双组分系统已被证明是金黄色葡萄球菌毒力的主要调节因子,但宿主环境对SaeR/S调控基因(SaeR/S靶标)的影响仍未完全明确。我们使用QuantiGene 2.0转录分析方法,检测了USA300中具有SaeR结合位点的基因在暴露于人和小鼠中性粒细胞、宿主来源的肽以及皮下皮肤感染期间的表达情况。我们发现,与整个SaeR/S毒力岛相反,只有部分SaeR/S靶标在与人中性粒细胞以及α-防御素相互作用的5分钟和10分钟内被激活。此外,尽管缺乏α-防御素,小鼠中性粒细胞仍能促进SaeR/S靶标的转录,并且小鼠皮肤环境引发了SaeR/S靶标独特的表达谱。这些发现表明,SaeR/S介导的转录对于特定宿主刺激具有独特性且依赖于特定宿主刺激。通过使用同基因的USA300ΔsaeR/S和USA300Δagr敲除菌株,我们还确定SaeR/S是毒力因子的主要调节因子,而群体感应双组分系统Agr在测试的生理条件下对SaeR/S靶标的转录有适度影响。

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