Platelet-derived growth factor-dependent association of the GTPase-activating protein of Ras and Src

Here we report that the platelet-derived growth factor beta preceptor (beta PDGFR) is not the only tyrosine kinase able to associate with the GTPase-activating protein of Ras (RasGAP). The interaction of non-beta PDGFR kinase(s) with RasGAP was dependent on stimulation with platelet-derived growth factor (PDGF) and seemed to require tyrosine phosphorylation of RasGAP. Because the tyrosine phosphorylation site of RasGAP is in a sequence context that is favoured by the Src homology 2 ('SH2') domain of Src family members, we tested the possibility that Src was the kinase that associated with RasGAP. Indeed, Src interacted with phosphorylated RasGAP fusion proteins; immunodepletion of Src markedly decreased the recovery of the RasGAP-associated kinase activity. Thus PDGF-dependent tyrosine phosphorylation of RasGAP results in the formation of a complex between RasGAP and Src. To begin to address the relevance of these observations, we focused on the consequences of the interaction of Src and RasGAP. We found that a receptor mutant that did not activate Src was unable to efficiently mediate the tyrosine phosphorylation of phospholipase C gamma (PLC gamma). Taken together, these observations support the following hypothesis. When RasGAP is recruited to the beta PDGFR, it is phosphorylated and associates with Src. Once bound to RasGAP, Src is no longer able to promote the phosphorylation of PLC gamma. This hypothesis offers a mechanistic explanation for our previously published findings that the recruitment of RasGAP to the beta PDGFR attenuates the tyrosine phosphorylation of PLC gamma. Finally, these findings suggest a novel way in which RasGAP negatively regulates signal relay by the beta PDGFR.