Journal article
Optic atrophy–associated TMEM126A is an assembly factor for the ND4-module of mitochondrial complex I
LE Formosa, B Reljic, AJ Sharpe, DH Hock, L Muellner-Wong, DA Stroud, MT Ryan
Proceedings of the National Academy of Sciences of the United States of America | Published : 2021
Abstract
Mitochondrial disease is a debilitating condition with a diverse genetic etiology. Here, we report that TMEM126A, a protein that is mutated in patients with autosomal-recessive optic atrophy, participates directly in the assembly of mitochondrial complex I. Using a combination of genome editing, interaction studies, and quantitative proteomics, we find that loss of TMEM126A results in an isolated complex I deficiency and that TMEM126A interacts with a number of complex I subunits and assembly factors. Pulse-labeling interaction studies reveal that TMEM126A associates with the newly synthesized mitochondrial DNA (mtDNA)-encoded ND4 subunit of complex I. Our findings indicate that TMEM126A is ..
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Grants
Awarded by National Health and Medical Research Council
Funding Acknowledgements
We thank the Bio21 Mass Spectrometry and Proteomics Facility and the Monash Proteomics and Metabolomics Facility for the provision of instrumentation, training, and technical support and Monash Flowcore for cell sorting. We acknowledge funding from the National Health and Medical Research Council (NHMRC Project Grants 1164459 and 1165217 to M.T.R.; 1125390 to M.T.R. and D.A.S.; NHMRC Fellowship 1140851 to D.A.S.).