A novel recognition motif for phosphatidylinositol 3-kinase binding mediates its association with the hepatocyte growth factor/scatter factor receptor.

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Mol Cell Biol. 1993 August; 13(8): 4600-4608

A novel recognition motif for phosphatidylinositol 3-kinase binding mediates its association with the hepatocyte growth factor/scatter factor receptor.

C Ponzetto, A Bardelli, F Maina, P Longati, G Panayotou, R Dhand, M D Waterfield and P M Comoglio

Department of Biomedical Sciences and Oncology, University of Turin, Italy.

ABSTRACT

The pleiotropic effects (mitogenesis, motogenesis, and morphogenesis)elicited by hepatocyte growth factor/scatter factor (HGF/SF)are mediated by the activation of the tyrosine kinase receptorencoded by the MET proto-oncogene. Following autophosphorylation,the receptor associates with the p85/110 phosphatidylinositol(PI) 3-kinase complex in vivo and in vitro. By a combinationof two complementary approaches, competition with syntheticphosphopeptides and association with Tyr-Phe receptor mutants,we have identified Y-1349 and Y-1356 in the HGF/SF receptoras the binding sites for PI 3-kinase. Y-1349VHV and Y-1356VNVdo not conform to the canonical consensus sequence YXXM forPI 3-kinase binding and thus define YVXV as a novel recognitionmotif. Y-1349 and Y-1356 are located within the C-terminal portionof the HGF/SF receptor and are phosphorylation sites. The affinityof the N- and C-terminal src homology region 2 (SH2) domainsof p85 for the phosphopeptides including Y-1349 and Y-1356 is2 orders of magnitude lower than that measured for Y-751 inthe platelet-derived growth factor receptor binding site. However,the closely spaced duplication of the novel recognition motifin the native HGF/SF receptor may allow binding with both SH2domains of p85, thus generating an efficient docking site forPI 3-kinase. In agreement with this model, we have observedthat a phosphopeptide including both Y-1349 and Y-1356 activatesPI 3-kinase in vitro.

Mol Cell Biol. 1993 August; 13(8): 4600-4608

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