拉布
内体
内吞循环
细胞生物学
效应器
胞浆
GTP酶
生物
化学
内吞作用
生物化学
细胞
细胞内
酶
作者
Wenjuan Zhang,Shimin Wang,Chao Yang,Can Hu,Dan Chen,Qian Luo,Zhen He,Yuhan Liao,Yuxin Yao,Juan Chen,Jun He,Junbo Hu,Tian Xia,Long Lin,Anbing Shi
出处
期刊:Cell Reports
[Elsevier]
日期:2020-09-01
卷期号:32 (12): 108173-108173
被引量:8
标识
DOI:10.1016/j.celrep.2020.108173
摘要
To explore the mechanism of Rab5/RAB-5 activation during endocytic recycling, we perform a genome-wide RNAi screen and identify a recycling regulator, LET-502/ROCK. LET-502 preferentially interacts with RAB-5(GDP) and activates RABX-5 GEF activity toward RAB-5, presumably by disrupting the self-inhibiting conformation of RABX-5. Furthermore, we find that the concomitant loss of LET-502 and another CED-10 effector, TBC-2/RAB-5-GAP, results in an endosomal buildup of RAB-5, indicating that CED-10 directs TBC-2-mediated RAB-5 inactivation and re-activates RAB-5 via LET-502 afterward. Then, we compare the functional position of LET-502 with that of RME-6/RAB-5-GEF. Loss of LET-502-RABX-5 module or RME-6 leads to diminished RAB-5 presence in spatially distinct endosome groups. We conclude that in the intestine of C. elegans, RAB-5 resides in discrete endosome subpopulations. Under the oversight of CED-10, LET-502 synergizes with RABX-5 to revitalize RAB-5 on a subset of endosomes in the deep cytosol, ensuring the progress of basolateral recycling.
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