Involvement of Shc in insulin- and epidermal growth factor-induced activation of p21ras.

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Mol Cell Biol. 1994 March; 14(3): 1575-1581

Involvement of Shc in insulin- and epidermal growth factor-induced activation of p21ras.

G J Pronk, A M de Vries-Smits, L Buday, J Downward, J A Maassen, R H Medema and J L Bos

Laboratory for Physiological Chemistry, Utrecht University, The Netherlands.

ABSTRACT

Shc proteins are phosphorylated on tyrosine residues and associatewith growth factor receptor-bound protein 2 (Grb2) upon treatmentof cells with epidermal growth factor (EGF) or insulin. We havestudied the role of Shc in insulin- and EGF-induced activationof p21ras in NIH 3T3 cells overexpressing human insulin receptors(A14 cells). A14 cells are equally responsive to insulin andEGF with respect to activation of p21ras. Analysis of Shc immunoprecipitatesrevealed that (i) both insulin and EGF treatment resulted inShc tyrosine phosphorylation and (ii) Shc antibodies coimmunoprecipitatedboth Grb2 and mSOS after insulin and EGF treatment. The inductionof tyrosine phosphorylation of Shc and the presence of Grb2and mSOS in Shc immunoprecipitates followed similar time courses,with somewhat higher levels after EGF treatment. In mSOS immunoprecipitates,Shc could be detected as well. Furthermore, Shc immune complexescontained guanine nucleotide exchange activity toward p21rasin vitro. From these results, we conclude that after insulinand EGF treatment, Shc associates with both Grb2 and mSOS andtherefore may mediate, at least in part, insulin- and EGF-inducedactivation of p21ras. In addition, we investigated whether theGrb2-mSOS complex associates with the insulin receptor or withinsulin receptor substrate 1 (IRS1). Although we observed associationof Grb2 with IRS1, we did not detect complex formation betweenmSOS and IRS1 in experiments in which the association of mSOSwith Shc was readily detectable. Furthermore, whereas EGF treatmentresulted in the association of mSOS with the EGF receptor, insulintreatment did not result in the association of mSOS with theinsulin receptor. These results indicate that the associationof Grb2-nSOS with Shc may be an important event in insulin-induced,mSOS-mediated activation of p21ras.

Mol Cell Biol. 1994 March; 14(3): 1575-1581

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