Mitochondrial matrix RTN4IP1/OPA10 is an oxidoreductase for coenzyme Q synthesis

Author:

Park Isaac,Kim Kwang-eunORCID,Kim Jeesoo,Kim Ae-Kyeong,Bae Subin,Jung Minkyo,Choi Jinhyuk,Mishra Pratyush KumarORCID,Kim Taek-Min,Kwak Chulhwan,Kang Myeong-Gyun,Yoo Chang-Mo,Mun Ji Young,Liu Kwang-Hyeon,Lee Kyu-SunORCID,Kim Jong-SeoORCID,Suh Jae MyoungORCID,Rhee Hyun-WooORCID

Abstract

AbstractTargeting proximity-labeling enzymes to specific cellular locations is a viable strategy for profiling subcellular proteomes. Here, we generated transgenic mice (MAX-Tg) expressing a mitochondrial matrix-targeted ascorbate peroxidase. Comparative analysis of matrix proteomes from the muscle tissues showed differential enrichment of mitochondrial proteins. We found that reticulon 4-interacting protein 1 (RTN4IP1), also known as optic atrophy-10, is enriched in the mitochondrial matrix of muscle tissues and is an NADPH oxidoreductase. Interactome analysis and in vitro enzymatic assays revealed an essential role for RTN4IP1 in coenzyme Q (CoQ) biosynthesis by regulating the O-methylation activity of COQ3. Rtn4ip1-knockout myoblasts had markedly decreased CoQ9 levels and impaired cellular respiration. Furthermore, muscle-specific knockdown of dRtn4ip1 in flies resulted in impaired muscle function, which was reversed by dietary supplementation with soluble CoQ. Collectively, these results demonstrate that RTN4IP1 is a mitochondrial NAD(P)H oxidoreductase essential for supporting mitochondrial respiration activity in the muscle tissue.

Publisher

Springer Science and Business Media LLC

Subject

Cell Biology,Molecular Biology

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