The tyrosine kinase encoded by the MET proto-oncogene is activated by autophosphorylation.

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Mol Cell Biol. 1991 April; 11(4): 1793-1803

The tyrosine kinase encoded by the MET proto-oncogene is activated by autophosphorylation.

L Naldini, E Vigna, R Ferracini, P Longati, L Gandino, M Prat and P M Comoglio

Department of Biomedical Sciences and Human Oncology, University of Turin Medical School, Italy.

ABSTRACT

Protein tyrosine kinases are crucially involved in the controlof cell proliferation. Therefore, the regulation of their activityin both normal and neoplastic cells has been under intense scrutiny.The product of the MET oncogene is a transmembrane receptorliketyrosine kinase with a unique disulfide-linked heterodimericstructure. Here we show that the tyrosine kinase activity ofthe MET-encoded protein is powerfully activated by tyrosineautophosphorylation. The enhancement of activity was quantitatedwith a phosphorylation assay of exogenous substrates. It involvedan increase in the Vmax of the enzyme-catalyzed phosphotransferreaction. No change was observed in the Km (substrate). A causalrelationship between tyrosine autophosphorylation and activationof the kinase activity was proved by (i) the kinetic agreementbetween autophosphorylation and kinase activation, (ii) theoverlapping dose-response relationship for ATP, (iii) the specificityfor ATP of the activation process, (iv) the phosphorylationof tyrosine residues only, in the Met protein, in the activationstep, (v) the linear dependence of the activation from the inputof enzyme assayed, and (vi) the reversal of the active stateby phosphatase treatment. Autophosphorylation occurred predominantlyon a single tryptic peptide, most likely via an intermolecularreaction. The structural features responsible for this positivemodulation of kinase activity were all contained in the 45-kDaintracellular moiety of the Met protein.

Mol Cell Biol. 1991 April; 11(4): 1793-1803

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