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一种受DNA损伤调节的含BRCT结构域蛋白TopBP1是细胞存活所必需的。

A DNA damage-regulated BRCT-containing protein, TopBP1, is required for cell survival.

作者信息

Yamane Kazuhiko, Wu Xianglin, Chen Junjie

机构信息

Division of Oncology Research, Mayo Clinic, Rochester, Minnesota 55905, USA.

出版信息

Mol Cell Biol. 2002 Jan;22(2):555-66. doi: 10.1128/MCB.22.2.555-566.2002.

DOI:10.1128/MCB.22.2.555-566.2002
PMID:11756551
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC139754/
Abstract

BRCA1 carboxyl-terminal (BRCT) motifs are present in a number of proteins involved in DNA repair and/or DNA damage-signaling pathways. Human DNA topoisomerase II binding protein 1 (TopBP1) contains eight BRCT motifs and shares sequence similarity with the fission yeast Rad4/Cut5 protein and the budding yeast DPB11 protein, both of which are required for DNA damage and/or replication checkpoint controls. We report here that TopBP1 is phosphorylated in response to DNA double-strand breaks and replication blocks. TopBP1 forms nuclear foci and localizes to the sites of DNA damage or the arrested replication forks. In response to DNA strand breaks, TopBP1 phosphorylation depends on the ataxia telangiectasia mutated protein (ATM) in vivo. However, ATM-dependent phosphorylation of TopBP1 does not appear to be required for focus formation following DNA damage. Instead, focus formation relies on one of the BRCT motifs, BRCT5, in TopBP1. Antisense Morpholino oligomers against TopBP1 greatly reduced TopBP1 expression in vivo. Similar to that of ataxia telangiectasia-related protein (ATR), Chk1, or Hus1, downregulation of TopBP1 leads to reduced cell survival, probably due to increased apoptosis. Taken together, the data presented here suggest that, like its putative counterparts in yeast species, TopBP1 may be involved in DNA damage and replication checkpoint controls.

摘要

BRCA1羧基末端(BRCT)基序存在于许多参与DNA修复和/或DNA损伤信号通路的蛋白质中。人类DNA拓扑异构酶II结合蛋白1(TopBP1)含有八个BRCT基序,与裂殖酵母Rad4/Cut5蛋白和芽殖酵母DPB11蛋白具有序列相似性,这两种蛋白都是DNA损伤和/或复制检查点控制所必需的。我们在此报告,TopBP1会因DNA双链断裂和复制阻滞而发生磷酸化。TopBP1形成核灶,并定位于DNA损伤部位或停滞的复制叉处。在响应DNA链断裂时,TopBP1的磷酸化在体内依赖于共济失调毛细血管扩张突变蛋白(ATM)。然而,DNA损伤后形成核灶似乎并不需要ATM依赖的TopBP1磷酸化。相反,核灶的形成依赖于TopBP1中的一个BRCT基序BRCT5。针对TopBP1的反义吗啉代寡聚物在体内大大降低了TopBP1的表达。与共济失调毛细血管扩张症相关蛋白(ATR)、Chk1或Hus1类似,TopBP1的下调导致细胞存活率降低,这可能是由于细胞凋亡增加所致。综上所述,本文提供的数据表明,与酵母中的假定对应物一样,TopBP1可能参与DNA损伤和复制检查点控制。

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