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伴侣蛋白协助的选择性自噬对于肌肉维持是必需的。

Chaperone-assisted selective autophagy is essential for muscle maintenance.

机构信息

Institute for Cell Biology and Bonner Forum Biomedizin, University of Bonn, Ulrich-Haberland-Strasse 61a, D-53121 Bonn, Germany.

出版信息

Curr Biol. 2010 Jan 26;20(2):143-8. doi: 10.1016/j.cub.2009.11.022. Epub 2010 Jan 7.

DOI:10.1016/j.cub.2009.11.022
PMID:20060297
Abstract

How are biological structures maintained in a cellular environment that constantly threatens protein integrity? Here we elucidate proteostasis mechanisms affecting the Z disk, a protein assembly essential for actin anchoring in striated muscles, which is subjected to mechanical, thermal, and oxidative stress during contraction [1]. Based on the characterization of the Drosophila melanogaster cochaperone Starvin (Stv), we define a conserved chaperone machinery required for Z disk maintenance. Instead of keeping Z disk proteins in a folded conformation, this machinery facilitates the degradation of damaged components, such as filamin, through chaperone-assisted selective autophagy (CASA). Stv and its mammalian ortholog BAG-3 coordinate the activity of Hsc70 and the small heat shock protein HspB8 during disposal that is initiated by the chaperone-associated ubiquitin ligase CHIP and the autophagic ubiquitin adaptor p62. CASA is thus distinct from chaperone-mediated autophagy, previously shown to facilitate the ubiquitin-independent, direct translocation of a client across the lysosomal membrane [2]. Impaired CASA results in Z disk disintegration and progressive muscle weakness in flies, mice, and men. Our findings reveal the importance of chaperone-assisted degradation for the preservation of cellular structures and identify muscle as a tissue that highly relies on an intact proteostasis network, thereby shedding light on diverse myopathies and aging.

摘要

在不断威胁蛋白质完整性的细胞环境中,生物结构是如何维持的?在这里,我们阐明了影响 Z 盘的蛋白质稳定机制,Z 盘是横纹肌中肌动蛋白锚定所必需的蛋白质组装体,在收缩过程中会受到机械、热和氧化应激的影响[1]。基于对果蝇 cochaperone Starvin(Stv)的特性的研究,我们定义了一个保守的伴侣蛋白机器,该机器对于 Z 盘的维持是必需的。与保持 Z 盘蛋白的折叠构象不同,该机器通过伴侣蛋白辅助的选择性自噬(CASA)促进了受损成分(如细丝蛋白)的降解。Stv 及其哺乳动物同源物 BAG-3 在由伴侣蛋白相关泛素连接酶 CHIP 和自噬泛素衔接蛋白 p62 启动的处置过程中协调 Hsc70 和小分子热休克蛋白 HspB8 的活性。因此,CASA 有别于先前显示可促进无泛素依赖性、直接将客户蛋白转运穿过溶酶体膜的伴侣蛋白介导的自噬[2]。CASA 的受损导致 Z 盘解体,并导致果蝇、小鼠和人类的肌肉逐渐虚弱。我们的发现揭示了伴侣蛋白辅助降解对于细胞结构的保存的重要性,并确定肌肉是高度依赖完整蛋白质稳定网络的组织,从而为各种肌肉疾病和衰老提供了新的认识。

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