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The Alternative Pathway of Glutathione Degradation Is Mediated by a Novel Protein Complex Involving Three New Genes in Saccharomyces cerevisiae

机译:谷胱甘肽降解的另一种途径是由涉及三个新基因的酿酒酵母的新型蛋白质复合体介导的。

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摘要

Glutathione (GSH), l-γ-glutamyl-l-cysteinyl-glycine, is the major low-molecular-weight thiol compound present in almost all eukaryotic cells. GSH degradation proceeds through the γ-glutamyl cycle that is initiated, in all organisms, by the action of γ-glutamyl transpeptidase. A novel pathway for the degradation of GSH that requires the participation of three previously uncharacterized genes is described in the yeast Saccharomyces cerevisiae. These genes have been named DUG1 (YFR044c), DUG2 (YBR281c), and DUG3 (YNL191w) (defective in utilization of glutathione). Although dipeptides and tripeptides with a normal peptide bond such as cys-gly or glu-cys-gly required the presence of only a functional DUG1 gene that encoded a protein belonging to the M20A metallohydrolase family, the presence of an unusual peptide bond such as in the dipeptide, γ-glu-cys, or in GSH, required the participation of the DUG2 and DUG3 gene products as well. The DUG2 gene encodes a protein with a peptidase domain and a large WD40 repeat region, while the DUG3 gene encoded a protein with a glutamine amidotransferase domain. The Dug1p, Dug2p, and Dug3p proteins were found to form a degradosomal complex through Dug1p–Dug2p and Dug2p–Dug3p interactions. A model is proposed for the functioning of the Dug1p/Dug2p/Dug3p proteins as a specific GSH degradosomal complex.
机译:谷胱甘肽(GSH)是一种1-γ-谷氨酰基-1-半胱氨酸-甘氨酸,是几乎所有真核细胞中都存在的主要低分子量硫醇化合物。 GSH降解通过γ-谷氨酰循环进行,该循环在所有生物体中都是通过γ-谷氨酰转肽酶的作用引发的。酵母酿酒酵母中描述了需要三个以前未表征的基因参与的GSH降解的新途径。这些基因已被命名为DUG1(YFR044c),DUG2(YBR281c)和DUG3(YNL191w)(在利用谷胱甘肽方面有缺陷)。尽管具有正常肽键的二肽和三肽(例如cys-gly或glu-cys-gly)仅需要存在一个功能性DUG1基因,该基因编码属于M20A金属水解酶家族的蛋白质,但存在一个不寻常的肽键,例如二肽γ-glu-cys或GSH中也需要DUG2和DUG3基因产物的参与。 DUG2基因编码具有肽酶结构域和较大的WD40重复区域的蛋白质,而DUG3基因编码具有谷氨酰胺酰胺转移酶结构域的蛋白质。发现Dug1p,Dug2p和Dug3p蛋白通过Dug1p–Dug2p和Dug2p–Dug3p相互作用形成了降解体复合物。提出了Dug1p / Dug2p / Dug3p蛋白作为特定的GSH降解体复合物的功能模型。

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