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A pathogenic cytochrome b mutation reveals new interactions between subunits of the mitochondrial bc1 complex
Authors:Saint-Georges Yann  Bonnefoy Nathalie  di Rago Jean Paul  Chiron Stephane  Dujardin Geneviève
Affiliation:Centre de Génétique Moléculaire du CNRS, Avenue de la Terrasse, 91198-Gif sur Yvette, France.
Abstract:Energy transduction in mitochondria involves five oligomeric complexes embedded within the inner membrane. They are composed of catalytic and noncatalytic subunits, the role of these latter proteins often being difficult to assign. One of these complexes, the bc1 complex, is composed of three catalytic subunits including cytochrome b and seven or eight noncatalytic subunits. Recently, several mutations in the human cytochrome b gene have been linked to various diseases. We have studied in detail the effects of a cardiomyopathy generating mutation G252D in yeast. This mutation disturbs the biogenesis of the bc1 complex at 36 degrees C and decreases the steady-state level of the noncatalytic subunit Qcr9p. In addition, the G252D mutation and the deletion of QCR9 show synergetic defects that can be partially bypassed by suppressor mutations at position 252 and by a new cytochrome b mutation, P174T. Altogether, our results suggest that the supernumerary subunit Qcr9p enhances or stabilizes the interactions between the catalytic subunits, this role being essential at high temperature.
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