Journal article

Mfn2 ubiquitination by PINK1/parkin gates the p97-dependent release of ER from mitochondria to drive mitophagy

GL McLelland, T Goiran, W Yi, G Dorval, CX Chen, ND Lauinger, AI Krahn, S Valimehr, A Rakovic, I Rouiller, TM Durcan, JF Trempe, EA Fon

Elife | ELIFE SCIENCES PUBLICATIONS LTD | Published : 2018

DOI: 10.7554/eLife.32866

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Abstract

Despite their importance as signaling hubs, the function of mitochondria-ER contact sites in mitochondrial quality control pathways remains unexplored. Here we describe a mechanism by which Mfn2, a mitochondria-ER tether, gates the autophagic turnover of mitochondria by PINK1 and parkin. Mitochondria-ER appositions are destroyed during mitophagy, and reducing mitochondria-ER contacts increases the rate of mitochondrial degradation. Mechanistically, parkin/ PINK1 catalyze a rapid burst of Mfn2 phosphoubiquitination to trigger p97-dependent disassembly of Mfn2 complexes from the outer mitochondrial membrane, dissociating mitochondria from the ER. We additionally demonstrate that a major portio..

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University of Melbourne Researchers

Grants

Funding Acknowledgements

Canadian Institutes of Health Research Canada Graduate Scholarship Gian-Luca McLellandCanadian Institutes of Health Research Foundation Grant Edward A Fon

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Keywords

1.1 Normal Biological Development and Functioning
Endoplasmic-Reticulum
Phosphorylated Ubiquitin
Autophagy
Cell Biology
3101 Biochemistry and Cell Biology
Activation
Parkinson'S Disease
Science & Technology
Snare Syntaxin 17
Parkinsons-Disease
Contact Site
Midbrain Dopamine Neurons
Complex
Biology
Mitofusin 2
Pink1
31 Biological Sciences
Life Sciences & Biomedicine
Life Sciences & Biomedicine - Other Topics
Human