| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 10869999 | FEBS Letters | 2015 | 8 Pages |
Abstract
The transient interactions of respiratory cytochrome c with complexes III and IV is herein investigated by using heterologous proteins, namely human cytochrome c, the soluble domain of plant cytochrome c1 and bovine cytochrome c oxidase. The binding molecular mechanisms of the resulting cross-complexes have been analyzed by Nuclear Magnetic Resonance and Isothermal Titration Calorimetry. Our data reveal that the two cytochrome c-involving adducts possess a 2:1 stoichiometry - that is, two cytochrome c molecules per adduct - at low ionic strength. We conclude that such extra binding sites at the surfaces of complexes III and IV can facilitate the turnover and sliding of cytochrome c molecules and, therefore, the electron transfer within respiratory supercomplexes.
Keywords
DLScytochrome C1(IV)CC1Cytochrome bc1HSQCCCOITCSupercomplexIMSPCCCSPnuclear magnetic resonanceHCCPCAelectron transferimmPrincipal component analysisNMRequilibrium dissociation constantinner mitochondrial membranecytochrome ccytochrome c oxidaseLuria-BertaniMitochondrial matrixComplex IVheteronuclear single-quantum correlationDynamic Light Scatteringcomplex IIIIsothermal titration calorimetry
Related Topics
Life Sciences
Agricultural and Biological Sciences
Plant Science
Authors
Blas Moreno-Beltrán, Irene DÃaz-Moreno, Katiuska González-Arzola, Alejandra Guerra-Castellano, Adrián Velázquez-Campoy, Miguel A. De la Rosa, Antonio DÃaz-Quintana,