首页> 美国卫生研究院文献>Journal of Bacteriology >Tricksy Business: Transcriptome Analysis Reveals the Involvement of Thioredoxin A in Redox Homeostasis Oxidative Stress Sulfur Metabolism and Cellular Differentiation in Bacillus subtilis
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Tricksy Business: Transcriptome Analysis Reveals the Involvement of Thioredoxin A in Redox Homeostasis Oxidative Stress Sulfur Metabolism and Cellular Differentiation in Bacillus subtilis

机译:cks琐的业务:转录组分析揭示了硫氧还蛋白A参与氧化还原稳态氧化应激硫代谢和枯草芽孢杆菌的细胞分化。

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摘要

Thioredoxins are important thiol-reactive proteins. Most knowledge about this class of proteins is derived from proteome studies, and little is known about the global transcriptional response of cells to various thioredoxin levels. In Bacillus subtilis, thioredoxin A is encoded by trxA and is essential for viability. In this study, we report the effects of minimal induction of a strain carrying an IPTG (isopropyl-β-d-thiogalactopyranoside)-inducible trxA gene (ItrxA) on transcription levels, as determined by DNA macroarrays. The effective depletion of thioredoxin A leads to the induction of genes involved in the oxidative stress response (but not those dependent on PerR), phage-related functions, and sulfur utilization. Also, several stationary-phase processes, such as sporulation and competence, are affected. The majority of these phenotypes are rescued by a higher induction level of ItrxA, leading to an approximately wild-type level of thioredoxin A protein. A comparison with other studies shows that the effects of thioredoxin depletion are distinct from, but show some similarity to, oxidative stress and disulfide stress. Some of the transcriptional effects may be linked to thioredoxin-interacting proteins. Finally, thioredoxin-linked processes appear to be conserved between prokaryotes and eukaryotes.
机译:硫氧还蛋白是重要的硫醇反应蛋白。关于此类蛋白质的大多数知识都来自蛋白质组学研究,而对于细胞对各种硫氧还蛋白水平的全局转录反应了解甚少。在枯草芽孢杆菌中,硫氧还蛋白A由trxA编码,对生存力至关重要。在这项研究中,我们报告了由IPTG(异丙基-β-d-硫代吡喃半乳糖吡喃糖苷)可诱导的trxA基因(ItrxA)引起的菌株的最小诱导对转录水平的影响,这是通过DNA宏阵列测定的。硫氧还蛋白A的有效耗竭导致诱导了参与氧化应激反应的基因(但不依赖于PerR的基因),噬菌体相关功能和硫的利用。此外,还会影响几个固定相过程,例如孢子形成和能力。这些表型中的大多数通过较高的ItrxA诱导水平得到挽救,从而导致硫氧还蛋白A蛋白的水平接近野生型。与其他研究的比较表明,硫氧还蛋白消耗的影响与氧化应激和二硫键应激不同,但显示出一些相似性。一些转录作用可能与硫氧还蛋白相互作用蛋白有关。最后,硫氧还蛋白连接的过程似乎在原核生物和真核生物之间是保守的。

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