1. MET phosphorylation predicts poor outcome in small cell lung carcinoma and its inhibition blocks HGF-induced effects in MET mutant cell lines.
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Arriola, E., Cañadas, I., Arumí-Uría, M., Dómine, M., Lopez-Vilariño, J. A., Arpí, O., Salido, M., Menéndez, S., Grande, E., Hirsch, F. R., Serrano, S., Bellosillo, B., Rojo, F., Rovira, A., Albanell, J., Cañadas, I, Arumí-Uría, M, Dómine, M, Lopez-Vilariño, J A, and Arpí, O
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PHOSPHORYLATION , *SMALL cell lung cancer , *GROWTH factors , *PROGNOSIS , *HEALTH outcome assessment , *CELL lines , *GENETICS - Abstract
Background: Small cell lung carcinoma (SCLC) has poor prognosis and remains orphan from targeted therapy. MET is activated in several tumour types and may be a promising therapeutic target.Methods: To evaluate the role of MET in SCLC, MET gene status and protein expression were evaluated in a panel of SCLC cell lines. The MET inhibitor PHA-665752 was used to study effects of pathway inhibition in basal and hepatocyte growth factor (HGF)-stimulated conditions. Immunohistochemistry for MET and p-MET was performed in human SCLC samples and association with outcome was assessed.Results: In MET mutant SCLC cells, HGF induced MET phosphorylation, increased proliferation, invasiveness and clonogenic growth. PHA-665752 blocked MET phosphorylation and counteracted HGF-induced effects. In clinical samples, total MET and p-MET overexpression were detected in 54% and 43% SCLC tumours (n = 77), respectively. MET phosphorylation was associated with poor median overall survival (132 days) vs p-MET negative cases (287 days) (P < 0.001). Phospho-MET retained its prognostic value in a multivariate analysis.Conclusions: MET activation resulted in a more aggressive phenotype in MET mutant SCLC cells and its inhibition by PHA-665752 reversed this phenotype. In patients with SCLC, MET activation was associated with worse prognosis, suggesting a role in the adverse clinical behaviour in this disease. [ABSTRACT FROM AUTHOR]- Published
- 2011
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