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帕金森病相关 DJ-1 的芽殖酵母直系同源物是一种多应激反应蛋白,可保护细胞免受毒性糖酵解产物的侵害。

The budding yeast orthologue of Parkinson's disease-associated DJ-1 is a multi-stress response protein protecting cells against toxic glycolytic products.

机构信息

Institute of Biochemistry and Biophysics, Polish Academy of Sciences, Pawińskiego 5A, 02-106 Warszawa, Poland.

Institute of Biochemistry and Biophysics, Polish Academy of Sciences, Pawińskiego 5A, 02-106 Warszawa, Poland.

出版信息

Biochim Biophys Acta Mol Cell Res. 2017 Jan;1864(1):39-50. doi: 10.1016/j.bbamcr.2016.10.016. Epub 2016 Oct 27.

DOI:10.1016/j.bbamcr.2016.10.016
PMID:27984092
Abstract

Saccharomyces cerevisiae Hsp31p is a DJ-1/ThiJ/PfpI family protein that was previously shown to be important for survival in the stationary phase of growth and under oxidative stress. Recently, it was identified as a chaperone or as glutathione-independent glyoxalase. To elucidate the role played by this protein in budding yeast cells, we investigated its involvement in the protection against diverse environmental stresses. Our study revealed that HSP31 gene expression is controlled by multiple transcription factors, including Yap1p, Cad1p, Msn2p, Msn4p, Haa1p and Hsf1p. These transcription factors mediate the HSP31 promoter responses to oxidative, osmotic and thermal stresses, to potentially toxic products of glycolysis, such as methylglyoxal and acetic acid, and to the diauxic shift. We also demonstrated that the absence of the HSP31 gene sensitizes cells to these stressors. Overproduction of Hsp31p and its homologue Hsp32p rescued the sensitivity of glo1Δ cells to methylglyoxal. Hsp31p also reversed the increased sensitivity of the ald6Δ strain to acetic acid. Since Hsp31p glyoxalase III coexists in S. cerevisiae cells with thousand-fold more potent glyoxalase I/II system, its biological purpose requires substantiation. We postulate that S. cerevisiae Hsp31p may have broader substrate specificity than previously proposed and is able to eliminate various toxic products of glycolysis. Alternatively, Hsp31p might be effective under high concentration of exogenous methylglyoxal present in some natural environmental niches populated by budding yeast, when glyoxalase I/II system capacity is saturated.

摘要

酿酒酵母 Hsp31p 是一种 DJ-1/ThiJ/PfpI 家族蛋白,先前研究表明它在生长静止期和氧化应激下的生存中起着重要作用。最近,它被鉴定为伴侣蛋白或谷胱甘肽非依赖性甘油醛酶。为了阐明该蛋白在出芽酵母细胞中的作用,我们研究了其在抵抗各种环境应激中的作用。我们的研究表明,HSP31 基因的表达受到多种转录因子的调控,包括 Yap1p、Cad1p、Msn2p、Msn4p、Haa1p 和 Hsf1p。这些转录因子介导 HSP31 启动子对氧化、渗透和热应激、糖酵解潜在毒性产物(如甲基乙二醛和乙酸)以及双相转换的反应。我们还证明,HSP31 基因的缺失使细胞对这些应激源敏感。Hsp31p 和其同源物 Hsp32p 的过表达挽救了 glo1Δ 细胞对甲基乙二醛的敏感性。Hsp31p 还逆转了 ald6Δ 菌株对乙酸的敏感性增加。由于 Hsp31p 甘油醛酶 III 与 S. cerevisiae 细胞中的千倍更强的甘油醛酶 I/II 系统共存,因此其生物学目的需要证实。我们推测,S. cerevisiae Hsp31p 可能具有比以前提出的更广泛的底物特异性,并且能够消除糖酵解的各种毒性产物。或者,当外源甲基乙二醛在某些自然环境小生境中存在高浓度时,Hsp31p 可能在糖酵解 I/II 系统能力饱和时有效,这些小生境由出芽酵母占据。

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