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Vps8 overexpression inhibits HOPS-dependent trafficking routes by outcompeting Vps41/Lt

机译:Vps8过表达通过与Vps41 / Lt竞争而抑制了HOPS依赖的贩运路线

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摘要

Two related multisubunit tethering complexes promote endolysosomal trafficking in all eukaryotes: Rab5-binding CORVET that was suggested to transform into Rab7-binding HOPS. We have previously identified miniCORVET, containing Drosophila Vps8 and three shared core proteins, which are required for endosome maturation upstream of HOPS in highly endocytic cells (Lőrincz et al., 2016a). Here, we show that Vps8 overexpression inhibits HOPS-dependent trafficking routes including late endosome maturation, autophagosome-lysosome fusion, crinophagy and lysosome-related organelle formation. Mechanistically, Vps8 overexpression abolishes the late endosomal localization of HOPS-specific Vps41/Lt and prevents HOPS assembly. Proper ratio of Vps8 to Vps41 is thus critical because Vps8 negatively regulates HOPS by outcompeting Vps41. Endosomal recruitment of miniCORVET- or HOPS-specific subunits requires proper complex assembly, and Vps8/miniCORVET is dispensable for autophagy, crinophagy and lysosomal biogenesis. These data together indicate the recruitment of these complexes to target membranes independent of each other in Drosophila, rather than their transformation during vesicle maturation.
机译:两种相关的多亚基束缚复合物可促进所有真核生物的溶酶体运输:结合Rab5的CORVET被建议转变为结合Rab7的HOPS。我们之前已经鉴定出miniCORVET,它含有果蝇Vps8和三个共有的核心蛋白,这是高度内吞细胞HOPS上游内体成熟所必需的(Lőrincz等人,2016a)。在这里,我们显示Vps8过表达抑制HOPS依赖的运输途径,包括晚期内体成熟,自噬体与溶酶体融合,吞噬和溶酶体相关细胞器的形成。从机制上讲,Vps8的过表达消除了HOPS特异性Vps41 / Lt的晚期内体定位,并阻止了HOPS组装。因此,Vps8与Vps41的正确比例至关重要,因为Vps8通过与Vps41竞争而对HOPS产生负向调节。内体募集miniCORVET或HOPS特异的亚基需要适当的复杂装配,而Vps8 / miniCORVET对于自噬,鼻咽癌和溶酶体生物发生是必不可少的。这些数据一起表明这些复合物在果蝇中彼此独立地募集到靶膜,而不是在囊泡成熟过程中转化。

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