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Biological and Pathological Implications of an Alternative ATP-Powered Proteasomal Assembly With Cdc48 and the 20S Peptidase

机译:具有Cdc48和20S肽酶的另一种ATP驱动的蛋白酶体组装的生物学和病理学意义。

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摘要

The ATP-powered protein degradation machinery plays essential roles in maintaining protein homeostasis in all organisms. Robust proteolytic activities are typically sequestered within protein complexes to avoid the fatal removal of essential proteins. Because the openings of proteolytic chambers are narrow, substrate proteins must undergo unfolding. AAA superfamily proteins (ATPases associated with diverse cellular activities) are mostly located at these openings and regulate protein degradation appropriately. The 26S proteasome, comprising 20S peptidase and 19S regulatory particles, is the major ATP-powered protein degradation machinery in eukaryotes. The 19S particles are composed of six AAA proteins and 13 regulatory proteins, and bind to both ends of a barrel-shaped proteolytic chamber formed by the 20S peptidase. Several recent studies have reported that another AAA protein, Cdc48, can replace the 19S particles to form an alternative ATP-powered proteasomal complex, i.e., the Cdc48-20S proteasome. This review focuses on our current knowledge of this alternative proteasome and its possible linkage to amyotrophic lateral sclerosis.
机译:由ATP驱动的蛋白质降解机制在维持所有生物体的蛋白质稳态中起着至关重要的作用。强大的蛋白水解活性通常被隔离在蛋白质复合物中,以避免致命性蛋白质的致命去除。由于蛋白水解室的开口狭窄,因此底物蛋白质必须经过折叠。 AAA超家族蛋白(与多种细胞活动相关的ATPase)大多位于这些开口处,并适当调节蛋白降解。包含20S肽酶和19S调节颗粒的26S蛋白酶体是真核生物中由ATP驱动的主要蛋白质降解机制。 19S颗粒由6种AAA蛋白和13种调节蛋白组成,并与20S肽酶形成的桶形蛋白水解室的两端结合。最近的几项研究报道说,另一种AAA蛋白Cdc48可以代替19S颗粒,形成另一种由ATP驱动的蛋白酶体复合物,即Cdc48-20S蛋白酶体。这项审查侧重于我们目前对这种替代蛋白酶体及其可能与肌萎缩性侧索硬化的联系的认识。

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