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酿酒酵母的DNA修复突变体pso2对双硫仑介导的乙醛脱氢酶抑制作用所积累的细胞内乙醛敏感。

DNA repair mutant pso2 of Saccharomyces cerevisiae is sensitive to intracellular acetaldehyde accumulated by disulfiram-mediated inhibition of acetaldehyde dehydrogenase.

作者信息

Brendel M, Marisco G, Ganda I, Wolter R, Pungartnik C

机构信息

Pós-Graduação em Genética e Biologia Molecular, Universidade Estadual de Santa Cruz, Ilhéus, BA, Brasil.

出版信息

Genet Mol Res. 2010 Jan 12;9(1):48-57. doi: 10.4238/vol9-1gmr695.

Abstract

Blocking aldehyde dehydrogenase with the drug disulfiram leads to an accumulation of intracellular acetaldehyde, which negatively affects the viability of the yeast Saccharomyces cerevisiae. Mutants of the yeast gene PSO2, which encodes a protein specific for repair of DNA interstrand cross-links, showed higher sensitivity to disulfiram compared to the wild type. This leads us to suggest that accumulated acetaldehyde induces DNA lesions, including highly deleterious interstrand cross-links. Acetaldehyde induced the expression of a PSO2-lacZ reporter construct that is specifically inducible by bi- or poly-functional mutagens, e.g., nitrogen mustard and photo-activated psoralens. Chronic exposure of yeast cells to disulfiram and acute exposure to acetaldehyde induced forward mutagenesis in the yeast CAN1 gene. Disulfiram-induced mutability of a pso2Delta mutant was significantly increased over that of the isogenic wild type; however, this was not found for acetaldehyde-induced mutagenesis. Spontaneous mutability at the CAN1 locus was elevated in pso2Delta, suggesting that growth of glucose-repressed yeast produces DNA lesions that, in the absence of Pso2p-mediated crosslink repair, are partially removed by an error-prone DNA repair mechanism. The use of disulfiram in the control of human alcohol abuse increases cellular acetaldehyde pools, which, based on our observations, enhances the risk of mutagenesis and of other genetic damage.

摘要

用药物双硫仑阻断乙醛脱氢酶会导致细胞内乙醛积累,这对酿酒酵母的活力产生负面影响。酵母基因PSO2的突变体编码一种特异性修复DNA链间交联的蛋白质,与野生型相比,该突变体对双硫仑表现出更高的敏感性。这使我们推测,积累的乙醛会诱导DNA损伤,包括高度有害的链间交联。乙醛诱导了PSO2 - lacZ报告基因构建体的表达,该构建体可被双功能或多官能诱变剂特异性诱导,例如氮芥和光活化补骨脂素。酵母细胞长期暴露于双硫仑以及急性暴露于乙醛会诱导酵母CAN1基因发生正向诱变。双硫仑诱导的pso2Δ突变体的突变率比同基因野生型显著增加;然而,乙醛诱导的诱变未发现这种情况。CAN1位点的自发突变率在pso2Δ中升高,这表明葡萄糖抑制的酵母生长会产生DNA损伤,在缺乏Pso2p介导的交联修复的情况下,这些损伤会被一种易出错的DNA修复机制部分去除。在控制人类酒精滥用中使用双硫仑会增加细胞内乙醛池,根据我们的观察,这会增加诱变和其他遗传损伤的风险。

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