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DNA damage modulates nucleolar interaction of the Werner protein with the AAA ATPase p97/VCP

机译:DNA损伤调节Werner蛋白与AAA ATPase p97 / VCP的核仁相互作用

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We report a novel nucleolar interaction between the AAA ATPase p97/VCP and the Werner protein (WRNp), a member of the RecQ helicase family. p97/VCP mediates several important cellular functions in eucaryotic cells, including membrane fusion of the endoplasmic reticulum and Golgi and ubiquitin-dependent protein degradation. Mutations in the WRN gene cause Werner syndrome, a genetic disorder characterized by premature onset of aging symptoms, a higher incidence of cancer, and a high susceptibility to DNA damage caused by topoisomerase inhibitors. We observed that both WRNp and valosin-containing protein (VCP) were present in the nucleoplasm and in nucleolar foci in mammalian cells and that WRNp and p97/VCP physically interacted in the nucleoli. Importantly, the nucleolar WRNp/VCP complex was dissociated by treatment with camptothecin, an inhibitor of topoisomerase 1, whereas other WRNp-associated protein complexes, such as WRNp/Ku 80, were not dissociated by this drug. Because WRN syndrome cells are sensitive to topoisomerase inhibitors, these observations suggest that the VCP/WRNp interaction plays an important role in WRN biology. We propose a novel role for VCP in the DNA damage response pathway through modulation of WRNp availability. [References: 67]
机译:我们报告了AAA ATPase p97 / VCP和Werner蛋白(WRNp),RecQ解旋酶家族成员之间的新型核仁相互作用。 p97 / VCP在真核细胞中介导了几种重要的细胞功能,包括内质网和高尔基体的膜融合以及泛素依赖性蛋白降解。 WRN基因中的突变会导致Werner综合征,Werner综合征是一种遗传性疾病,其特征是过早出现衰老症状,较高的癌症发病率以及对拓扑异构酶抑制剂引起的DNA损伤的高度敏感性。我们观察到WRNp和含valosin的蛋白质(VCP)都存在于哺乳动物细胞的核质和核仁病灶中,并且WRNp和p97 / VCP在核仁中发生物理相互作用。重要的是,核苷WRNp / VCP复合物通过喜树碱(拓扑异构酶1的抑制剂)处理而解离,而其他WRNp相关蛋白复合物(例如WRNp / Ku 80)并未被该药物解离。由于WRN综合征细胞对拓扑异构酶抑制剂敏感,因此这些发现表明VCP / WRNp相互作用在WRN生物学中起着重要作用。我们提出VCP通过调节WRNp可用性在DNA损伤反应途径中的新作用。 [参考:67]

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