Abstract
The Met tyrosine kinase – the HGF receptor – induces cell transformation and metastasis when constitutively activated. Met signaling is mediated by phosphorylation of two carboxy-terminal tyrosines which act as docking sites for a number of SH2-containing molecules. These include Grb2 and p85 which couple the receptor, respectively, with Ras and PI 3-kinase. We previously showed that a Met mutant designed to obtain preferential coupling with Grb2 (Met2xGrb2) is permissive for motility, increases transformation, but – surprisingly – is impaired in causing invasion and metastasis. In this work we used Met mutants optimized for binding either p85 alone (Met2xPI3K) or p85 and Grb2 (MetP13K/Grb2) to evaluate the relative importance of Ras and PI 3-kinase as downstream effectors of Met. Met2xPI3K was competent in eliciting motility, but not transformation, invasion, or metastasis. Conversely, MetP13K/Grb2 induced motility, transformation, invasion and metastasis as efficiently as wild type Met. Furthermore, the expression of constitutively active PI 3-kinase in cells transformed by the Met2xGrb2 mutant, fully rescued their ability to invade and metastasize. These data point to a central role for PI 3-kinase in Met-mediated invasiveness, and indicate that simultaneous activation of Ras and PI 3-kinase is required to unleash the Met metastatic potential.
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Acknowledgements
We thank Flavio Maina for part of the original mutagenesis work. This research was supported by grants from the Associazione Italiana delle Ricerche sul Cancro (AIRC to CP and PMC). CP gratefully acknowledges the continuing support of the Compagnia di San Paolo and Fondazione CRT to her laboratory.
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Bardelli, A., Basile, M., Audero, E. et al. Concomitant activation of pathways downstream of Grb2 and PI 3-kinase is required for MET-mediated metastasis. Oncogene 18, 1139–1146 (1999). https://doi.org/10.1038/sj.onc.1202607
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DOI: https://doi.org/10.1038/sj.onc.1202607
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