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Ag43的相变与OxyR的氧化状态无关。

Phase variation of Ag43 is independent of the oxidation state of OxyR.

作者信息

Wallecha Anu, Correnti Jason, Munster Vincent, van der Woude Marjan

机构信息

Department of Microbiology, University of Pennsylvania, Philadelphia, Pennsylvania 19104, USA.

出版信息

J Bacteriol. 2003 Apr;185(7):2203-9. doi: 10.1128/JB.185.7.2203-2209.2003.

Abstract

OxyR is a DNA binding protein that differentially regulates a cell's response to hydrogen peroxide-mediated oxidative stress. We previously reported that the reduced form of OxyR is sufficient for repression of transcription of agn43 from unmethylated template DNA, which is essential for deoxyadenosine methylase (Dam)- and OxyR-dependent phase variation of agn43. Here we provide evidence that the oxidized form of OxyR [OxyR(ox)] also represses agn43 transcription. In vivo, we found that exogenous addition of hydrogen peroxide, sufficient to oxidize OxyR, did not affect the expression of agn43. OxyR(ox) repressed in vitro transcription but only from an unmethylated agn43 template. The -10 sequence of the promoter and three Dam target sequences were protected in an in vitro DNase I footprint assay by OxyR(ox). Furthermore, OxyR(ox) bound to the agn43 regulatory region DNA with an affinity similar to that for the regulatory regions of katG and oxyS, which are activated by OxyR(ox), indicating that binding at agn43 can occur at biologically relevant concentrations. OxyR-dependent regulation of Ag43 expression is therefore unusual in firstly that OxyR binding at agn43 is dependent on the methylation state of Dam target sequences in its binding site and secondly that OxyR-dependent repression appears to be independent of hydrogen-peroxide mediated oxidative stress and the oxidation state of OxyR.

摘要

OxyR是一种DNA结合蛋白,它以不同方式调节细胞对过氧化氢介导的氧化应激反应。我们之前报道过,OxyR的还原形式足以抑制未甲基化模板DNA上agn43的转录,这对于agn43依赖脱氧腺苷甲基化酶(Dam)和OxyR的相变至关重要。在此我们提供证据表明,OxyR的氧化形式[OxyR(ox)]也能抑制agn43的转录。在体内,我们发现外源添加足以氧化OxyR的过氧化氢并不影响agn43的表达。OxyR(ox)抑制体外转录,但仅抑制未甲基化的agn43模板的转录。在体外DNase I足迹实验中,OxyR(ox)保护了启动子的-10序列和三个Dam靶序列。此外,OxyR(ox)与agn43调控区DNA的结合亲和力与它对被OxyR(ox)激活的katG和oxyS调控区的结合亲和力相似,这表明在生理相关浓度下,OxyR(ox)能与agn43结合。因此,OxyR对Ag43表达的调控具有独特之处,首先,OxyR在agn43上的结合取决于其结合位点中Dam靶序列的甲基化状态;其次,OxyR依赖的抑制作用似乎独立于过氧化氢介导的氧化应激以及OxyR的氧化状态。

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