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CORVET 和 HOPS 衔接复合物——内体和溶酶体融合的协调者。

CORVET and HOPS tethering complexes - coordinators of endosome and lysosome fusion.

机构信息

University of Osnabrück, Department of Biology/Chemistry, Biochemistry Section, Barbarastrasse 13, 49076 Osnabrück, Germany.

出版信息

J Cell Sci. 2013 Mar 15;126(Pt 6):1307-16. doi: 10.1242/jcs.107805.

Abstract

Protein and lipid transport along the endolysosomal system of eukaryotic cells depends on multiple fusion and fission events. Over the past few years, the molecular constituents of both fission and fusion machineries have been identified. Here, we focus on the mechanism of membrane fusion at endosomes, vacuoles and lysosomes, and in particular on the role of the two homologous tethering complexes called CORVET and HOPS. Both complexes are heterohexamers; they share four subunits, interact with Rab GTPases and soluble NSF attachment protein receptors (SNAREs) and can tether membranes. Owing to the presence of specific subunits, CORVET is a Rab5 effector complex, whereas HOPS can bind efficiently to late endosomes and lysosomes through Rab7. Based on the recently described overall structure of the HOPS complex and a number of in vivo and in vitro analyses, important insights into their function have been obtained. Here, we discuss the general function of both complexes in yeast and in metazoan cells in the context of endosomal biogenesis and maturation.

摘要

真核细胞的内体溶酶体系统中的蛋白质和脂质运输依赖于多种融合和裂变事件。在过去的几年中,已经鉴定出了裂变和融合机制的多种分子成分。在这里,我们专注于内体、液泡和溶酶体中膜融合的机制,特别是同源牵带复合物 CORVET 和 HOPS 的作用。这两个复合物都是异六聚体;它们共享四个亚基,与 Rab GTPases 和可溶性 NSF 附着蛋白受体 (SNAREs) 相互作用,并可以连接膜。由于存在特定的亚基,CORVET 是 Rab5 效应复合物,而 HOPS 可以通过 Rab7 有效地与晚期内体和溶酶体结合。基于最近描述的 HOPS 复合物的整体结构和许多体内和体外分析,已经获得了它们功能的重要见解。在这里,我们讨论了这两个复合物在酵母和后生动物细胞中的一般功能,涉及内体发生和成熟。

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