The Vps39-like TRAP1 is an effector of Rab5 and likely the missing Vps3 subunit of human CORVET.

Cellular logistics Pub Date : 2014-10-02 eCollection Date: 2014-10-01 DOI:10.4161/21592780.2014.970840
Jens Lachmann, Elina Glaubke, Patrick S Moore, Christian Ungermann
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引用次数: 29

Abstract

Membrane fusion in the endocytic pathway is mediated by a protein machinery consistent of Rab GTPases, tethering factors and SNAREs. In yeast, the endosomal CORVET and lysosomal HOPS tethering complexes share 4 of their 6 subunits. The 2 additional subunits in each complex - Vps3 and Vps8 for CORVET, and the homologous Vps39 and Vps41 for HOPS - bind directly to Rab5 and Rab7, respectively. In humans, all subunits for HOPS have been described. However, human CORVET remains poorly characterized and a homolog of Vps3 is still missing. Here we characterize 2 previously identified Vps39 isoforms, hVps39-1/hVam6/TLP and hVps39-2/TRAP1, in yeast and HEK293 cells. None of them can compensate the loss of the endogenous yeast Vps39, though the specific interaction of hVps39-1 with the virus-specific LT protein was reproduced. Both human Vps39 proteins show a cytosolic localization in yeast and mammalian cells. However, hVps39-2/TRAP1 strongly co-localizes with co-expressed Rab5 and interacts directly with Rab5-GTP in vitro. We conclude that hVps39-2/TRAP1 is an endosomal protein and an effector of Rab5, suggesting a role of the protein as a subunit of the putative human CORVET complex.

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vps39样的TRAP1是Rab5的效应物,可能是人类CORVET缺失的Vps3亚基。
内吞途径中的膜融合是由一种蛋白质机制介导的,这种机制与Rab GTPases、系住因子和SNAREs一致。在酵母菌中,内体的CORVET和溶酶体的啤酒花捆绑复合物在6个亚基中有4个是相同的。每个复合物中的2个附加亚基- CORVET的Vps3和Vps8,以及HOPS的同源Vps39和Vps41 -分别直接与Rab5和Rab7结合。在人类中,已经描述了啤酒花的所有亚基。然而,人类CORVET的特征仍然很差,vp3的同源物仍然缺失。我们在酵母和HEK293细胞中鉴定了2种先前鉴定的Vps39亚型,hvs39 -1/hVam6/TLP和hvs39 -2/TRAP1。它们都不能弥补内源性酵母Vps39的损失,尽管hVps39-1与病毒特异性LT蛋白的特异性相互作用被复制。两种人类Vps39蛋白在酵母和哺乳动物细胞中都有胞质定位。然而,hVps39-2/TRAP1与共表达的Rab5强共定位,并直接与Rab5- gtp在体外相互作用。我们得出结论,hVps39-2/TRAP1是一种内体蛋白和Rab5的效应蛋白,表明该蛋白作为假定的人类CORVET复合体的一个亚基发挥作用。
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