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Wrestling with stress: Roles of protein SUMOylation and deSUMOylation in cell stress response

机译:与压力搏斗:蛋白质SUMO化和去SUMO化在细胞应激反应中的作用

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摘要

How cell fate is determined following extreme stress is a core question in cell biology. This is particularly important in the brain where neuronal death following ischemic stroke is a major cause of disability. Over the last few years it has emerged that the SUMOylation status of an increasing number of substrate proteins plays a crucial role in cellular responses to environmental and metabolic stress. SUMOylation is a post-translational modification in which the 97-residue protein, SUMO (Small Ubiquitin-related MOdifier) is covalently attached to specific lysine residues in a target protein. Despite being covalent, it is a highly transient modification because of the actions of deSUMOylation enzymes, so SUMO conjugation acts as a rapidly reversible switch that can promote or inhibit protein interactions with the substrate protein. Overall, it appears that increased SUMOylation represents a cellular protective response. Here we discuss recent progress toward understanding the mechanisms, pathways, and roles of SUMOylation during and after severe metabolic stress
机译:极端压力后如何确定细胞命运是细胞生物学的核心问题。这在缺血性中风后神经元死亡是致残的主要原因的大脑中尤其重要。在过去的几年中,已经发现越来越多的底物蛋白的SUMO化状态在细胞对环境和代谢应激的反应中起着至关重要的作用。 SUMOylation是一种翻译后修饰,其中97个残基的蛋白质SUMO(与泛素相关的小修饰子)共价连接至目标蛋白质中的特定赖氨酸残基。尽管是共价的,但由于deSUMOylation酶的作用,它是高度瞬时的修饰,因此SUMO共轭起着快速可逆的作用,可以促进或抑制蛋白质与底物蛋白质的相互作用。总体而言,似乎增加的SUMOylation代表细胞保护性反应。在这里,我们讨论了在理解严重代谢应激期间和之后SUMOylation的机制,途径和作用方面的最新进展。

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