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首页> 外文期刊>Nature cell biology >Reversible protein aggregation is a protective mechanism to ensure cell cycle restart after stress
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Reversible protein aggregation is a protective mechanism to ensure cell cycle restart after stress

机译:可逆蛋白质聚集是一种保护机制,以确保压力后的细胞周期重启

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摘要

Protein aggregation is mostly viewed as deleterious and irreversible causing several pathologies. However, reversible protein aggregation has recently emerged as a novel concept for cellular regulation. Here, we characterize stress-induced, reversible aggregation of yeast pyruvate kinase, Cdc19. Aggregation of Cdc19 is regulated by oligomerization and binding to allosteric regulators. We identify a region of low compositional complexity (LCR) within Cdc19 as necessary and sufficient for reversible aggregation. During exponential growth, shielding the LCR within tetrameric Cdc19 or phosphorylation of the LCR prevents unscheduled aggregation, while its dephosphorylation is necessary for reversible aggregation during stress. Cdc19 aggregation triggers its localization to stress granules and modulates their formation and dissolution. Reversible aggregation protects Cdc19 from stress-induced degradation, thereby allowing cell cycle restart after stress. Several other enzymes necessary for G1 progression also contain LCRs and aggregate reversibly during stress, implying that reversible aggregation represents a conserved mechanism regulating cell growth and survival.
机译:蛋白质聚集主要被视为有害和不可逆转的导致几种病理学。然而,可逆蛋白质聚集最近被出现为细胞调节的新概念。在这里,我们表征了酵母丙酮酸激酶,CDC19的应激诱导的可逆聚集。 CDC19的聚集通过寡聚化和结合颠促调节剂来调节。我们根据需要识别CDC19中的低组合物复合性(LCR)的区域,并且足以可逆聚集。在指数生长期间,在四聚体CDC19中屏蔽LCR或LCR的磷酸化防止非划分的聚集,而其去磷酸化是在压力期间可逆聚集所必需的。 CDC19聚集触发其定位对应力颗粒并调节它们的形成和溶解。可逆聚集可以保护CDC19免受应力诱导的降解,从而允许在应力后重启细胞周期。 G1进展所需的几种其他酶也含有LCRS和可逆地在应力期间聚集,这意味着可逆聚集是调节细胞生长和存活的保守机制。

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