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Drp1-Zip1 Interaction Regulates Mitochondrial Quality Surveillance System

Authors
Cho, Hyo MinRyu, Jae RyunJo, YouhwaSeo, Tae WoongChoi, Ye NaKim, June HoanChung, Jee MinCho, BongkiKang, Ho ChulYu, Seong-WoonYoo, Soon JiKim, HyunSun, Woong
Issue Date
17-Jan-2019
Publisher
CELL PRESS
Keywords
Drp1; mitochondrial fission; mitochondrial membrane potential; mitochondrial quality control; mitochondrial quality surveillance; mitophagy; Zip1
Citation
MOLECULAR CELL, v.73, no.2, pp.364 - +
Indexed
SCIE
SCOPUS
Journal Title
MOLECULAR CELL
Volume
73
Number
2
Start Page
364
End Page
+
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/68273
DOI
10.1016/j.molcel.2018.11.009
ISSN
1097-2765
Abstract
Mitophagy, a mitochondrial quality control process for eliminating dysfunctional mitochondria, can be induced by a response of dynamin-related protein 1 (Drp1) to a reduction in mitochondrial membrane potential (MMP) and mitochondrial division. However, the coordination between MMP and mitochondrial division for selecting the damaged portion of the mitochondrial network is less understood. Here, we found that MMP is reduced focally at a fission site by the Drp1 recruitment, which is initiated by the interaction of Drp1 with mitochondrial zinc transporter Zip1 and Zn2+ entry through the Zip1-MCU complex. After division, healthy mitochondria restore MMPlevels and participate in the fusion-fission cycle again, but mitochondria that fail to restore MMP undergo mitophagy. Thus, interfering with the interaction between Drp1 and Zip1 blocks the reduction of MMP and the subsequent mitophagic selection of damaged mitochondria. These results suggest that Drp1-dependent fission provides selective pressure for eliminating "bad sectors'' in the mitochondrial network, serving as a mitochondrial quality surveillance system.
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