| Literature DB >> 25959673 |
David Pacheu-Grau1, Bettina Bareth1, Jan Dudek1, Lisa Juris1, F-Nora Vögtle2, Mirjam Wissel1, Scot C Leary3, Sven Dennerlein1, Peter Rehling4, Markus Deckers1.
Abstract
Three mitochondria-encoded subunits form the catalytic core of cytochrome c oxidase, the terminal enzyme of the respiratory chain. COX1 and COX2 contain heme and copper redox centers, which are integrated during assembly of the enzyme. Defects in this process lead to an enzyme deficiency and manifest as mitochondrial disorders in humans. Here we demonstrate that COA6 is specifically required for COX2 biogenesis. Absence of COA6 leads to fast turnover of newly synthesized COX2 and a concomitant reduction in cytochrome c oxidase levels. COA6 interacts transiently with the copper-containing catalytic domain of newly synthesized COX2. Interestingly, similar to the copper metallochaperone SCO2, loss of COA6 causes cardiomyopathy in humans. We show that COA6 and SCO2 interact and that corresponding pathogenic mutations in each protein affect complex formation. Our analyses define COA6 as a constituent of the mitochondrial copper relay system, linking defects in COX2 metallation to cardiac cytochrome c oxidase deficiency.Entities:
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Year: 2015 PMID: 25959673 DOI: 10.1016/j.cmet.2015.04.012
Source DB: PubMed Journal: Cell Metab ISSN: 1550-4131 Impact factor: 27.287