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硫醇氧化还原蛋白质组学鉴定酿酒酵母细胞质和线粒体谷氧还蛋白-2同工型的差异靶标。DHBP 合酶(RIB3)的可逆 S-谷胱甘肽化。

Thiol redox proteomics identifies differential targets of cytosolic and mitochondrial glutaredoxin-2 isoforms in Saccharomyces cerevisiae. Reversible S-glutathionylation of DHBP synthase (RIB3).

机构信息

Department of Biochemistry and Molecular Biology, University of Córdoba and Córdoba Maimónides Institute for Biomedical Research, IMIBIC, Córdoba, Spain.

出版信息

J Proteomics. 2011 Oct 19;74(11):2487-97. doi: 10.1016/j.jprot.2011.04.018. Epub 2011 Apr 30.

DOI:10.1016/j.jprot.2011.04.018
PMID:21565288
Abstract

Yeast Grx2 plays a role in the antioxidant glutathione linked defense acting on the redox status of protein cysteines, but the exact action or its specificity is not known. Moreover, it localizes in cytosol and mitochondria where it can exert different functions. To search for functions of Grx2 we determined the differential "Thiolic Redox Proteome" of control and peroxide-treated yeast mutant cells lacking the gene for Grx2 or expressing Grx2 exclusively in the mitochondria. Forty-two proteins have been identified that have alternative redox oxidation states as a consequence of Grx2 absence from the cell or expression in the mitochondria and absence from the cytosol. The precise cysteine residues affected have been mapped for each protein. One target protein, Rib3p, which has as yet an undefined function in respiration, was confirmed to have its Cys56 reversibly S-glutathionylated in vitro in a Grx2p dependent process. Grx2-dependent redox changes in key enzymes of glutamate consuming amino acid biosynthetic pathways could favor glutathione biosynthesis. Other target proteins are involved in membrane fusion, cell wall structure and ribosome assembly, but others are of unknown function. These results provide clues on the metabolic hot spots of redox regulatory mechanisms.

摘要

酵母 Grx2 在与蛋白质半胱氨酸的氧化还原状态相关的抗氧化谷胱甘肽链接防御中发挥作用,但确切的作用或其特异性尚不清楚。此外,它定位于细胞质和线粒体中,在那里可以发挥不同的功能。为了寻找 Grx2 的功能,我们确定了对照和过氧化物处理的酵母突变细胞的差异“硫醇氧化还原蛋白质组”,这些细胞缺乏 Grx2 基因或仅在线粒体中表达 Grx2。已经鉴定出 42 种蛋白质,由于 Grx2 从细胞中缺失或在细胞质中表达而从线粒体中缺失,它们具有替代的氧化还原氧化状态。已经为每种蛋白质映射了受影响的确切半胱氨酸残基。一个靶蛋白 Rib3p 在呼吸中具有尚未定义的功能,其 Cys56 在体外的 Grx2p 依赖过程中被证实可被可逆 S-谷胱甘肽化。谷氨酸消耗氨基酸生物合成途径中的关键酶的 Grx2 依赖性氧化还原变化可能有利于谷胱甘肽的生物合成。其他靶蛋白参与膜融合、细胞壁结构和核糖体组装,但其他蛋白的功能未知。这些结果为氧化还原调节机制的代谢热点提供了线索。

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