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Hul5 泛素连接酶:清除坏蛋白。

Hul5 ubiquitin ligase: good riddance to bad proteins.

机构信息

Department of Biochemistry and Molecular Biology, University of British Columbia, Vancouver, Canada.

出版信息

Prion. 2012 Jul 1;6(3):240-4. doi: 10.4161/pri.19929.

Abstract

Failure to eliminate abnormal proteins in the cell is associated with numerous aggregation diseases. Misfolded proteins are normally detected by protein quality control and either refolded or eliminated. The ubiquitin-proteasome system is a major pathway that degrades these unwanted proteins. Ubiquitin ligases are central to these degradation pathways as they recognize aberrant proteins and covalently attach a polyubiquitin chain to target them to the proteasome. We discovered that the Hul5 ubiquitin ligase is a major player in a novel protein quality control pathway that targets cytosolic misfolded proteins. Hul5 is required for the maintenance of cell fitness and the increased ubiquitination of low solubility proteins after heat-shock in yeast cells. We identified several low-solubility substrates of Hul5, including the prion-like protein Pin3. It is now apparent that in the cytoplasm, misfolded proteins can be targeted by multiple degradation pathways. In this review, we discuss how the Hul5 protein quality control pathway may specifically target low solubility cytosolic proteins in the cell.

摘要

细胞中异常蛋白质的清除失败与许多聚集性疾病有关。错误折叠的蛋白质通常被蛋白质质量控制检测到,并被重新折叠或消除。泛素-蛋白酶体系统是降解这些不需要的蛋白质的主要途径。泛素连接酶是这些降解途径的核心,因为它们识别异常蛋白质,并将多聚泛素链共价连接到靶标上,将其靶向蛋白酶体。我们发现,Hul5 泛素连接酶是一种新型蛋白质质量控制途径的主要参与者,该途径靶向细胞质中错误折叠的蛋白质。Hul5 对于维持细胞活力以及在酵母细胞中热休克后低溶解度蛋白质的泛素化增加是必需的。我们鉴定了 Hul5 的几个低溶解度底物,包括朊病毒样蛋白 Pin3。现在很明显,在细胞质中,错误折叠的蛋白质可以被多种降解途径靶向。在这篇综述中,我们讨论了 Hul5 蛋白质质量控制途径如何特异性地靶向细胞中低溶解度的细胞质蛋白质。

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