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首页> 外文期刊>Molecular cell >A transcriptional activator is part of an SCF ubiquitin ligase to control degradation of its cofactors.
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A transcriptional activator is part of an SCF ubiquitin ligase to control degradation of its cofactors.

机译:转录激活因子是SCF泛素连接酶的一部分,可控制其辅因子的降解。

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摘要

Multisubunit protein complexes pose a challenge to the coordinated regulation of individual components. We show how the yeast transactivating factor Met4 functions as a component of the SCF(Met30) ubiquitin ligase to synchronize its own activity with cofactor assembly. Cells maintain Met4 in a dormant state by a regulatory ubiquitin chain assembled by SCF(Met30). Nutritional and heavy-metal stress block Met4 ubiquitylation resulting in Met4 activation, which induces a stress-response program including cell-cycle arrest. Met4 relies on assembly with various cofactors for promoter binding. We report here that the stability of these DNA-binding cofactors is regulated by SCF(Met30). Remarkably, the transcriptional activator Met4 functions as a substrate-specificity factor in the context of SCF(Met30/Met4) to coordinate cofactor degradation with its own activity status. Our results establish an additional layer for substrate recruitment by SCF ubiquitin ligases and provide conceptual insight into coordinated regulation of protein complexes.
机译:多亚基蛋白质复合物对单个成分的协调调控提出了挑战。我们展示了酵母反式激活因子Met4如何作为SCF(Met30)泛素连接酶的组成部分,以使其自身的活性与辅因子组装同步。细胞通过由SCF(Met30)组装的调控泛素链使Met4处于休眠状态。营养和重金属胁迫会阻止Met4泛素化,从而导致Met4激活,从而诱导应激反应程序,包括细胞周期停滞。 Met4依赖于各种与启动子结合的辅因子的组装。我们在这里报告,这些DNA结合辅因子的稳定性由SCF(Met30)调节。值得注意的是,转录激活因子Met4在SCF(Met30 / Met4)的背景下充当底物特异性因子,以协调辅因子降解与其自身的活性状态。我们的结果为SCF泛素连接酶为底物募集建立了新的一层,并为蛋白质复合物的协调调控提供了概念性见解。

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