Publication | Open Access
Formation of apoptosome is initiated by cytochrome <i>c</i> -induced dATP hydrolysis and subsequent nucleotide exchange on Apaf-1
330
Citations
28
References
2005
Year
Datp HydrolysisApoptosisMolecular BiologyCell DeathRedox BiologyOxidative StressAutophagySubsequent Nucleotide ExchangeProteomicsCell SignalingBiochemistryHorse HeartCytochrome CBiochemical InteractionCell BiologyProtein PhosphorylationSignal TransductionCellular EnzymologyMitochondrial FunctionNatural SciencesCellular BiochemistryMedicine
Apoptosis in metazoans is executed by a group of intracellular proteases named caspases. One of the caspase-activating pathways in mammals is initiated by the release of cytochrome c from mitochondria to cytosol, where it binds to Apaf-1 to form a procaspase-9-activating heptameric protein complex named apoptosome. We report here the reconstitution of this pathway with purified recombinant Apaf-1, procaspase-9, procaspase-3, and cytochrome c from horse heart. Apaf-1 contains a dATP as a cofactor. Cytochrome c binding to Apaf-1 induces hydrolysis of dATP to dADP, which is subsequently replaced by exogenous dATP. The dATP hydrolysis and exchange on Apaf-1 are two required steps for apoptosome formation.
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