| Literature DB >> 27050458 |
Ming Chen1,2, Ziheng Chen1,2, Yueying Wang1,2, Zheng Tan1,2, Chongzhuo Zhu1,2, Yanjun Li1,2, Zhe Han3, Linbo Chen3, Ruize Gao3, Lei Liu1,2, Quan Chen1,2,3.
Abstract
Mitochondrial fragmentation due to imbalanced fission and fusion of mitochondria is a prerequisite for mitophagy, however, the exact "coupling" of mitochondrial dynamics and mitophagy remains unclear. We have previously identified that FUNDC1 recruits MAP1LC3B/LC3B (LC3) through its LC3-interacting region (LIR) motif to initiate mitophagy in mammalian cells. Here, we show that FUNDC1 interacts with both DNM1L/DRP1 and OPA1 to coordinate mitochondrial fission or fusion and mitophagy. OPA1 interacted with FUNDC1 via its Lys70 (K70) residue, and mutation of K70 to Ala (A), but not to Arg (R), abolished the interaction and promoted mitochondrial fission and mitophagy. Mitochondrial stress such as selenite or FCCP treatment caused the disassembly of the FUNDC1-OPA1 complex while enhancing DNM1L recruitment to the mitochondria. Furthermore, we observed that dephosphorylation of FUNDC1 under stress conditions promotes the dissociation of FUNDC1 from OPA1 and association with DNM1L. Our data suggest that FUNDC1 regulates both mitochondrial fission or fusion and mitophagy and mediates the "coupling" across the double membrane for mitochondrial dynamics and quality control.Entities:
Keywords: DNM1L/DRP1; OPA1; mitochondrial dynamics; mitophagy; mitophagy receptor
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Year: 2016 PMID: 27050458 PMCID: PMC4836026 DOI: 10.1080/15548627.2016.1151580
Source DB: PubMed Journal: Autophagy ISSN: 1554-8627 Impact factor: 16.016