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J Biol Chem, Vol. 274, Issue 4, 1898-1904, January 22, 1999
From INSERM U428, Faculté de Pharmacie, Université
Paris-V, 75270 Paris, France
The platelet receptor for the Fc domain of IgGs
(Fc
RIIa) triggers intracellular signaling through protein tyrosine
phosphorylations leading to platelet aggregation. In this study, we
focused on the adaptor protein p120cbl (Cbl), which became
tyrosine-phosphorylated after platelet activation induced by
antibodies. Cbl phosphorylation was dependent on Fc receptor
engagement. An association of Cbl with the p85 subunit of
phosphatidylinositol 3-kinase (PI 3-K) occurred in parallel with Cbl
tyrosine phosphorylation. We showed by in vitro experiments that Cbl/p85 association was mediated by the Src homology 3 domain of
p85/PI 3-K and the proline-rich region of Cbl. Inhibition of PI 3-K
activity by wortmannin led to the blockade of both platelet aggregation
and serotonin release mediated by Fc
RIIa engagement, whereas it only
partly inhibited those induced by thrombin. Thus, PI 3-K may play a
crucial role in the initiation of platelet responses after Fc
RIIa
engagement. Our results suggest that Cbl is involved in platelet signal
transduction by the recruitment of PI 3-K to the Fc
RIIa pathway,
possibly by increasing PI 3-K activity.
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