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HIGD2A is Required for Assembly of the COX3 Module of Human Mitochondrial Complex IV

Daniella H. Hock, Boris Reljić, Ching‐Seng Ang, Linden Muellner-Wong, Hayley S. Mountford, Alison G. Compton, Michael T. Ryan, David R. Thorburn, David A. Stroud

2020Molecular & Cellular Proteomics59 citationsDOIOpen Access PDF

Abstract

biogenesis of mtDNA-encoded COX3, subsequent accumulation of complex IV intermediates and turnover of COX3 partner proteins. Deletion of HIGD2A also leads to defective complex IV activity. The impact of HIGD2A loss on complex IV was not altered by growth under hypoxic conditions, consistent with its role being in basal complex IV assembly. Although in the absence of HIGD2A we show that mitochondria do contain an altered supercomplex assembly, we demonstrate it to harbor a crippled complex IV lacking COX3. Our results redefine HIGD2A as a classical assembly factor required for building the COX3 module of complex IV.

Topics & Concepts

ChemistryComputational biologyComputer scienceCell biologyBiologyMitochondrial Function and PathologyATP Synthase and ATPases ResearchUbiquitin and proteasome pathways
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