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The N-Terminal Domains of Vps3 and Vps8 Are Critical for Localization and Function of the CORVET Tethering Complex on Endosomes

机译:Vps3和Vps8的N末端域对于CORVET束缚复合物在内体上的定位和功能至关重要

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摘要

Endosomal biogenesis depends on multiple fusion and fission events. For fusion, the heterohexameric CORVET complex as an effector of the endosomal Rab5/Vps21 GTPase has a central function in the initial tethering event. Here, we show that the CORVET-specific Vps3 and Vps8 subunits, which interact with Rab5/Vps21, require their N-terminal domains for localization and function. Surprisingly, CORVET may lack either one of the two N-terminal domains, but not both, to promote protein sorting via the endosome. The dually truncated complex mislocalizes to the cytosol and is impaired in endocytic protein sorting, but not in assembly. Furthermore, the endosomal localization can be rescued by overexpression of Vps21 or one of the truncated CORVET subunits, even though CORVET assembly is not impaired by loss of the N-terminal domains or in strains lacking all endosomal Rab5s and Ypt7. We thus conclude that CORVET requires only its C-terminal domains for assembly and has beyond its putative β-propeller domains additional binding sites for endosomes, which could be important to bind Vps21 and other endosome-specific factors for efficient endosome tethering.
机译:内体生物发生取决于多种融合和裂变事件。对于融合,作为内体Rab5 / Vps21 GTPase效应子的异六聚体CORVET复合物在最初的束缚事件中具有核心功能。在这里,我们显示与Rab5 / Vps21相互作用的CORVET特异的Vps3和Vps8亚基需要其N末端域才能定位和发挥功能。出人意料的是,CORVET可能缺少两个N末端结构域之一,但不是两个都无法促进通过内体的蛋白质分选。双重截短的复合物错位到细胞质,并在胞吞蛋白分选中受损,但在装配中没有受损。此外,即使CORVET装配不受N末端结构域的缺失或缺乏所有内体Rab5s和Ypt7的菌株的破坏,也可以通过Vps21或被截短的CORVET亚基之一的过表达来挽救内体定位。因此,我们得出结论,CORVET仅需要其C末端结构域进行组装,而在其推定的β-螺旋结构域之外还具有内体的其他结合位点,这对于结合Vps21和其他内体特异性因子进行有效的内体束缚可能很重要。

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