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Comparative Genomics of Thiol Oxidoreductases Reveals Widespread and Essential Functions of Thiol-based Redox Control of Cellular Processes

机译:硫醇氧化还原酶的比较基因组学揭示了基于硫醇的氧化还原控制细胞过程的广泛和基本功能。

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摘要

>Aims: Redox regulation of cellular processes is an important mechanism that operates in organisms from bacteria to mammals. Much of the redox control is provided by thiol oxidoreductases: proteins that employ cysteine residues for redox catalysis. We wanted to identify thiol oxidoreductases on a genome-wide scale and use this information to obtain insights into the general principles of thiol-based redox control. >Results: Thiol oxidoreductases were identified by three independent methods that took advantage of the occurrence of selenocysteine homologs of these proteins and functional linkages among thiol oxidoreductases revealed by comparative genomics. Based on these searches, we describe thioredoxomes, which are sets of thiol oxidoreductases in organisms. Their analyses revealed that these proteins are present in all living organisms, generally account for 0.5%–1% of the proteome and that their use correlates with proteome size, distinguishing these proteins from those involved in core metabolic functions. We further describe thioredoxomes of Saccharomyces cerevisiae and humans, including proteins which have not been characterized previously. Thiol oxidoreductases occur in various cellular compartments and are enriched in the endoplasmic reticulum and cytosol. >Innovation: We developed bioinformatics methods and used them to characterize thioredoxomes on a genome-wide scale, which in turn revealed properties of thioredoxomes. >Conclusion: These data provide information about organization and properties of thiol-based redox control, whose use is increased with the increase in complexity of organisms. Our data also show an essential combined function of a set of thiol oxidoreductases, and of thiol-based redox regulation in general, in all living organisms. Antioxid. Redox Signal. 16, 193–201.
机译:>目标:细胞过程的氧化还原调节是一种重要机制,可在从细菌到哺乳动物的生物体内发挥作用。大部分的氧化还原控制是由硫醇氧化还原酶提供的:巯基氧化还原酶利用半胱氨酸残基进行氧化还原催化。我们希望在全基因组范围内鉴定巯基氧化还原酶,并使用该信息来深入了解基于巯基的氧化还原控制的一般原理。 >结果:通过三种独立的方法鉴定了硫醇氧化还原酶,这些方法利用了这些蛋白质的硒代半胱氨酸同源物以及比较基因组学揭示的硫醇氧化还原酶之间的功能性连接。基于这些搜索,我们描述了硫氧化还原酶,它是生物体中的硫醇氧化还原酶集。他们的分析表明,这些蛋白质存在于所有活生物体中,通常占蛋白质组的0.5%–1%,并且它们的使用与蛋白质组大小相关,从而将这些蛋白质与参与核心代谢功能的蛋白质区分开。我们进一步描述了酿酒酵母和人的硫氧还酶基因组,包括以前未鉴定的蛋白质。硫醇氧化还原酶存在于各种细胞区室中,并且富含内质网和胞质溶胶。 >创新:我们开发了生物信息学方法,并用它们在全基因组范围内表征了硫氧还蛋白基因组,从而揭示了硫氧还蛋白基因组的特性。 >结论:这些数据提供了有关基于硫醇的氧化还原控制的组织和特性的信息,随着生物复杂性的增加,其使用量也在增加。我们的数据还显示了在所有活生物体中,一组硫醇氧化还原酶和基于硫醇的氧化还原调节的基本综合功能。抗氧化。氧化还原信号。 16,193–201。

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