Mitochondrial cytochrome c oxidase biogenesis: Recent developments

Timón Gómez, Alba; Nývltová, Eva; Abriata, Luciano Andres; Vila, Alejandro Jose; Hosler, Jonathan; Barrientos, Antoni

info:eu-repo/semantics/article

Fecha

2018-04

Registro en:

Timón Gómez, Alba; Nývltová, Eva; Abriata, Luciano Andres; Vila, Alejandro Jose; Hosler, Jonathan; et al.; Mitochondrial cytochrome c oxidase biogenesis: Recent developments; Academic Press Ltd - Elsevier Science Ltd; Seminars In Cell & Developmental Biology; 76; 4-2018; 163-178

1084-9521

http://hdl.handle.net/11336/94374

CONICET Digital

CONICET

https://repositorioslatinoamericanos.uchile.cl/handle/2250/4405768

Autor

Timón Gómez, Alba

Nývltová, Eva

Abriata, Luciano Andres

Vila, Alejandro Jose

Hosler, Jonathan

Barrientos, Antoni

Institución

Consejo Nacional de Investigaciones Científicas y Tecnológicas (Argentina)

Resumen

Mitochondrial cytochrome c oxidase (COX) is the primary site of cellular oxygen consumption and is essential for aerobic energy generation in the form of ATP. Human COX is a copper-heme A hetero-multimeric complex formed by 3 catalytic core subunits encoded in the mitochondrial DNA and 11 subunits encoded in the nuclear genome. Investigations over the last 50 years have progressively shed light into the sophistication surrounding COX biogenesis and the regulation of this process, disclosing multiple assembly factors, several redox-regulated processes leading to metal co-factor insertion, regulatory mechanisms to couple synthesis of COX subunits to COX assembly, and the incorporation of COX into respiratory supercomplexes. Here, we will critically summarize recent progress and controversies in several key aspects of COX biogenesis: linear versus modular assembly, the coupling of mitochondrial translation to COX assembly and COX assembly into respiratory supercomplexes.

Materias

COX ASSEMBLY FACTOR

COX1

COX2

MITOCHONDRIAL CYTOCHROME C OXIDASE

RESPIRATORY SUPERCOMPLEX

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