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USP17- and SCFβTrCP--regulated degradation of DEC1 controls the DNA damage response.

机译：由USP17和SCFβTrCP调控的DEC1降解控制DNA损伤反应。

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摘要

In response to genotoxic stress, DNA damage checkpoints maintain the integrity of the genome by delaying cell cycle progression to allow for DNA repair. Here we show that the degradation of the basic helix-loop-helix (bHLH) transcription factor DEC1, a critical regulator of cell fate and circadian rhythms, controls the DNA damage response. During unperturbed cell cycles, DEC1 is a highly unstable protein that is targeted for proteasome-dependent degradation by the SCF(βTrCP) ubiquitin ligase in cooperation with CK1. Upon DNA damage, DEC1 is rapidly induced in an ATM/ATR-dependent manner. DEC1 induction results from protein stabilization via a mechanism that requires the USP17 ubiquitin protease. USP17 binds and deubiquitylates DEC1, markedly extending its half-life. Subsequently, during checkpoint recovery, DEC1 proteolysis is reestablished through βTrCP-dependent ubiquitylation. Expression of a degradation-resistant DEC1 mutant prevents checkpoint recovery by inhibiting the downregulation of p53. These results indicate that the regulated degradation of DEC1 is a key factor controlling the DNA damage response.

机译：响应遗传毒性压力，DNA损伤检查点通过延迟细胞周期进程以允许DNA修复来维持基因组的完整性。在这里，我们表明基本螺旋-环-螺旋（bHLH）转录因子DEC1的降解，细胞命运和昼夜节律的关键调节器，控制DNA损伤反应。在不受干扰的细胞周期中，DEC1是高度不稳定的蛋白质，与CK1协同作用，可被SCF（βTrCP）泛素连接酶靶向蛋白酶体依赖性降解。 DNA受损后，以ATM / ATR依赖性方式迅速诱导DEC1。 DEC1诱导是通过需要USP17泛素蛋白酶的机制稳定蛋白质而产生的。 USP17结合并脱去泛素化DEC1，从而显着延长了其半衰期。随后，在检查点恢复期间，通过依赖于βTrCP的泛素化来重新建立DEC1蛋白水解。抗降解的DEC1突变体的表达通过抑制p53的下调来防止检查点恢复。这些结果表明，DEC1的受控降解是控制DNA损伤反应的关键因素。

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Kim, J; D'Annibale, S; Magliozzi, R; Low, TY; Jansen, P; Shaltiel, IA; Mohammed, S; Heck, AJ; Medema, RH; Guardavaccaro, D;
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1. USP17- and SCFβTrCP-Regulated Degradation of DEC1 Controls the DNA Damage Response [J] . Jihoon Kim, Sara DAnnibale, Roberto Magliozzi, Molecular and Cellular Biology . 2014,第22期

机译：USP17和SCFβTrCP调控的DEC1降解控制DNA损伤反应
2. Cisplatin sensitivity is related to late DNA damage processing and checkpoint control rather than to the early DNA damage response. [J] . Mutation Research: International Journal on Mutagenesis, Chromosome Breakage and Related Subjects . 2009,第1a2期

机译：顺铂敏感性与后期DNA损伤处理和检查点控制有关，而不与早期DNA损伤反应有关。
3. Phosphorylation and degradation of MdmX is inhibited by Wip1 phosphatase in the DNA damage response. [J] . Zhang X, Lin L, Guo H Cancer research: The official organ of the American Association for Cancer Research, Inc . 2009,第20期

机译：WIP1磷酸酶在DNA损伤反应中抑制MDMX的磷酸化和降解。
4. DNA and Estrogen Receptor Interaction Revealed by the Fragment Molecular Orbital Method - Implementation of SCF Convergence - [C] . T. Watanabe, Y. Inadomi, S. Tanaka, NSTI(Nano Science and Technology Institute) Nanotechnology Conference and Trade Show(Nanotech 2004) . 2004

机译：片段分子轨道法揭示DNA与雌激素受体的相互作用-SCF收敛的实现-
5. Cell cycle-regulated human DNA helicase B in DNA damage response. [D] . Gu, Jinming. 2005

机译：细胞周期调节的人类DNA解旋酶B在DNA损伤反应中。
6. USP17- and SCFβTrCP-Regulated Degradation of DEC1 Controls the DNA Damage Response [O] . Jihoon Kim, Sara DAnnibale, Roberto Magliozzi, 2014

机译：USP17和SCFβTrCP调控的DEC1降解控制DNA损伤反应
7. USP17- and SCFβTrCP--regulated degradation of DEC1 controls the DNA damage response [O] . Kim, Jihoon, D'Annibale, Sara, Magliozzi, Roberto, 2014

机译：USP17和SCFβTrCP调控的DEC1降解控制DNA损伤反应

USP17- and SCFβTrCP--regulated degradation of DEC1 controls the DNA damage response.

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