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金黄色葡萄球菌中 SarA 对硫氧还蛋白还原酶基因 (trxB) 转录的调控。

Control of thioredoxin reductase gene (trxB) transcription by SarA in Staphylococcus aureus.

机构信息

Division of Basic Biomedical Sciences, University of South Dakota, Sanford School of Medicine, 414 E Clark Street, Vermillion, SD 57069, USA.

出版信息

J Bacteriol. 2010 Jan;192(1):336-45. doi: 10.1128/JB.01202-09.

Abstract

Thioredoxin reductase (encoded by trxB) protects Staphylococcus aureus against oxygen or disulfide stress and is indispensable for growth. Among the different sarA family mutants analyzed, transcription of trxB was markedly elevated in the sarA mutant under conditions of aerobic as well as microaerophilic growth, indicating that SarA acts as a negative regulator of trxB expression. Gel shift analysis showed that purified SarA protein binds directly to the trxB promoter region DNA in vitro. DNA binding of SarA was essential for repression of trxB transcription in vivo in S. aureus. Northern blot analysis and DNA binding studies of the purified wild-type SarA and the mutant SarAC9G with oxidizing agents indicated that oxidation of Cys-9 reduced the binding of SarA to the trxB promoter DNA. Oxidizing agents, in particular diamide, could further enhance transcription of the trxB gene in the sarA mutant, suggesting the presence of a SarA-independent mode of trxB induction. Analysis of two oxidative stress-responsive sarA regulatory target genes, trxB and sodM, with various mutant sarA constructs showed a differential ability of the SarA to regulate expression of the two above-mentioned genes in vivo. The overall data demonstrate the important role played by SarA in modulating expression of genes involved in oxidative stress resistance in S. aureus.

摘要

硫氧还蛋白还原酶(由 trxB 编码)可保护金黄色葡萄球菌免受氧或二硫化物应激,并对其生长是不可或缺的。在所分析的不同 sarA 家族突变体中,在有氧和微需氧生长条件下,sarA 突变体中的 trxB 转录明显升高,表明 SarA 作为 trxB 表达的负调节剂。凝胶迁移分析表明,纯化的 SarA 蛋白可在体外直接结合 trxB 启动子区域 DNA。SarA 在体内 DNA 结合对于 trxB 转录的抑制是必需的。用氧化剂进行的 Northern blot 分析和对纯化的野生型 SarA 和突变体 SarAC9G 的 DNA 结合研究表明,Cys-9 的氧化降低了 SarA 与 trxB 启动子 DNA 的结合。氧化剂,特别是二酰胺,可进一步增强 sarA 突变体中 trxB 基因的转录,表明存在 SarA 非依赖性 trxB 诱导模式。用各种突变 sarA 构建体对两个氧化应激响应 sarA 调节靶基因 trxB 和 sodM 的分析表明,SarA 具有不同的能力来调节体内上述两个基因的表达。总的来说,这些数据表明 SarA 在调节金黄色葡萄球菌中参与氧化应激抗性的基因表达方面发挥了重要作用。

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