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Coordination of metal center biogenesis in human cytochrome c oxidase
Medicine and HealthNature Communications

Coordination of metal center biogenesis in human cytochrome c oxidase

E. Nývltová, J. V. Dietz, et al.

Discover groundbreaking insights into mitochondrial cytochrome c oxidase (CCO) and its copper chaperones in human cells, as explored by Eva Nývltová, Jonathan V. Dietz, Javier Seravalli, Oleh Khalimonchuk, and Antoni Barrientos. This research unveils mechanisms that control crucial biosynthesis processes, preventing harmful accumulation of reactive intermediates.... show more
Abstract
Mitochondrial cytochrome c oxidase (CCO) or respiratory chain complex IV is a heme a3-copper oxygen reductase containing metal centers essential for holo-complex biogenesis and enzymatic function that are assembled by subunit-specific metallochaperones. The enzyme has two copper sites located in the catalytic core subunits. The COX1 subunit harbors the CuB site that tightly associates with heme a3 while the COX2 subunit contains the binuclear CuA site. Here, we report that in human cells the CcO copper chaperones form macromolecular assemblies and cooperate with several twin CXC proteins to control heme a biosynthesis and coordinate copper transfer sequentially to the CuA and CuB sites. These data on CcO illustrate a mechanism that regulates the biogenesis of macromolecular enzymatic assemblies with several catalytic metal redox centers and prevents the accumulation of cytotoxic reactive assembly intermediates.
Publisher
Nature Communications
Published On
Jun 24, 2022
Authors
Eva Nývltová, Jonathan V. Dietz, Javier Seravalli, Oleh Khalimonchuk, Antoni Barrientos
Tags
cytochrome c oxidasecopper chaperonesheme a biosynthesismetal redox centersmacromolecular assemblies
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