首页> 外文期刊>Nucleic Acids Research >Ubiquitin ligase UBR3 regulates cellular levels of the essential DNA repair protein APE1 and is required for genome stability
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Ubiquitin ligase UBR3 regulates cellular levels of the essential DNA repair protein APE1 and is required for genome stability

机译:泛素连接酶UBR3调节基本DNA修复蛋白APE1的细胞水平,是基因组稳定所必需的

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APE1 (Ref-1) is an essential human protein involved in DNA damage repair and regulation of transcription. Although the cellular functions and biochemical properties of APE1 are well characterized, the mechanism involved in regulation of the cellular levels of this important DNA repair/transcriptional regulation enzyme, remains poorly understood. Using an in vitro ubiquitylation assay, we have now purified the human E3 ubiquitin ligase UBR3 as a major activity that polyubiquitylates APE1 at multiple lysine residues clustered on the N-terminal tail. We further show that a knockout of the Ubr3 gene in mouse embryonic fibroblasts leads to an up-regulation of the cellular levels of APE1 protein and subsequent genomic instability. These data propose an important role for UBR3 in the control of the steady state levels of APE1 and consequently error free DNA repair.
机译:APE1(Ref-1)是一种必需的人类蛋白质,参与DNA损伤修复和转录调控。尽管对APE1的细胞功能和生化特性进行了很好的表征,但对该重要DNA修复/转录调节酶的细胞水平调节所涉及的机制仍知之甚少。使用体外泛素化测定,我们现在纯化了人E3泛素连接酶UBR3,这是一种主要活性,可在N末端尾部上的多个赖氨酸残基上使APE1泛素化。我们进一步表明,在小鼠胚胎成纤维细胞中敲除Ubr3基因会导致APE1蛋白的细胞水平上调和随后的基因组不稳定。这些数据表明UBR3在控制APE1的稳态水平并因此实现无错DNA修复中起着重要作用。

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