Publication | Open Access
Identification of Protein Kinase Cα as an Essential, but Not Sufficient, Cytosolic Factor for Ca2+-induced α- and Dense-core Granule Secretion in Platelets
48
Citations
44
References
2001
Year
Protein SecretionPlatelet PathobiologyProtein Kinase CαCellular PhysiologyDense-core Granule SecretionSecretory GranulesWhereas PkcalphaCell SignalingCell PhysiologyMolecular PhysiologyProtein Kinase CalphaVascular BiologyMembrane BiologyGranule SecretionsPharmacologyCell BiologyProtein PhosphorylationSignal TransductionBlood PlateletPhysiologyCytosolic FactorCellular BiochemistryMedicine
Upon activation, platelets release many active substances. Here, we have analyzed the mechanism governing Ca(2+)-induced secretion of von Willebrand factor stored in alpha-granules and 5-hydroxytryptamine in dense-core granules in permeabilized human platelets. Both secretions were dependent on ATP and cytosol. An essential factor for both granule secretions was purified from rat brain cytosol and identified to be protein kinase Calpha (PKCalpha) by partial amino acid sequencing. Purified PKCalpha efficiently stimulated both secretions in the presence of cytosol, whereas PKCalpha alone did not support the secretion of either type of granules, suggesting that PKCalpha is not a sufficient factor. Finally, in human platelet cytosol fractionated by a gel filtration column, the stimulatory activity for dense-core granule secretion paralleled with the concentration of PKC, suggesting that PKC could also be such a stimulatory factor in platelet cytosol. Thus, we identified PKCalpha as an essential, but not sufficient, cytosolic factor for the Ca(2+)-induced secretions of both alpha- and dense-core granules in platelets.
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