| Literature DB >> 27588602 |
Zheng Wang1, Guangyan Miao2, Xue Xue1, Xiangyang Guo3, Chongzhen Yuan1, Zhaoyu Wang1, Gangming Zhang1, Yingyu Chen4, Du Feng5, Junjie Hu1, Hong Zhang6.
Abstract
Mutations in the human autophagy gene EPG5 cause the multisystem disorder Vici syndrome. Here we demonstrated that EPG5 is a Rab7 effector that determines the fusion specificity of autophagosomes with late endosomes/lysosomes. EPG5 is recruited to late endosomes/lysosomes by direct interaction with Rab7 and the late endosomal/lysosomal R-SNARE VAMP7/8. EPG5 also binds to LC3/LGG-1 (mammalian and C. elegans Atg8 homolog, respectively) and to assembled STX17-SNAP29 Qabc SNARE complexes on autophagosomes. EPG5 stabilizes and facilitates the assembly of STX17-SNAP29-VAMP7/8 trans-SNARE complexes, and promotes STX17-SNAP29-VAMP7-mediated fusion of reconstituted proteoliposomes. Loss of EPG5 activity causes abnormal fusion of autophagosomes with various endocytic vesicles, in part due to elevated assembly of STX17-SNAP25-VAMP8 complexes. SNAP25 knockdown partially suppresses the autophagy defect caused by EPG5 depletion. Our study reveals that EPG5 is a Rab7 effector involved in autophagosome maturation, providing insight into the molecular mechanism underlying Vici syndrome.Entities:
Keywords: LC3; RAB effector; SNARE; autophagosome maturation; epg-5
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Year: 2016 PMID: 27588602 DOI: 10.1016/j.molcel.2016.08.021
Source DB: PubMed Journal: Mol Cell ISSN: 1097-2765 Impact factor: 17.970