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Supercomplex assembly determines electron flux in the mitochondrial electron transport chain.

Science (New York, N.Y.) (2013-07-03)
Esther Lapuente-Brun, Raquel Moreno-Loshuertos, Rebeca Acín-Pérez, Ana Latorre-Pellicer, Carmen Colás, Eduardo Balsa, Ester Perales-Clemente, Pedro M Quirós, Enrique Calvo, M A Rodríguez-Hernández, Plácido Navas, Raquel Cruz, Ángel Carracedo, Carlos López-Otín, Acisclo Pérez-Martos, Patricio Fernández-Silva, Erika Fernández-Vizarra, José Antonio Enríquez
ABSTRACT

The textbook description of mitochondrial respiratory complexes (RCs) views them as free-moving entities linked by the mobile carriers coenzyme Q (CoQ) and cytochrome c (cyt c). This model (known as the fluid model) is challenged by the proposal that all RCs except complex II can associate in supercomplexes (SCs). The proposed SCs are the respirasome (complexes I, III, and IV), complexes I and III, and complexes III and IV. The role of SCs is unclear, and their existence is debated. By genetic modulation of interactions between complexes I and III and III and IV, we show that these associations define dedicated CoQ and cyt c pools and that SC assembly is dynamic and organizes electron flux to optimize the use of available substrates.

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Sigma-Aldrich
Citocromo c, ≥95% (SDS-PAGE)
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Citocromo c, ≥95% based on Mol. Wt. 12,327 basis
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Citocromo c, ≥95% based on Mol. Wt. 12,384 basis
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Citocromo c, ≥95% based on Mol. Wt. 12,327 basis, powder, suitable for mammalian cell culture
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Citocromo c, BioReagent, suitable for GFC marker
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Citocromo c, vial of 10 nmol, (M+H+) 12,361.96 Da by calculation
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