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  • Drug development of MET inhibitors: targeting oncogene addiction and expedience.

Drug development of MET inhibitors: targeting oncogene addiction and expedience.

Nature reviews. Drug discovery (2008-05-31)
Paolo M Comoglio, Silvia Giordano, Livio Trusolino
ABSTRACT

The MET tyrosine kinase stimulates cell scattering, invasion, protection from apoptosis and angiogenesis, thereby acting as a powerful expedient for cancer dissemination. MET can also be genetically selected for the long-term maintenance of the primary transformed phenotype, and some tumours appear to be dependent on (or 'addicted' to) sustained MET activity for their growth and survival. Because of its dual role as an adjuvant, pro-metastatic gene for some tumour types and as a necessary oncogene for others, MET is a versatile candidate for targeted therapeutic intervention. Here we discuss recent progress in the development of molecules that inhibit MET function and consider their application in a subset of human tumours that are potentially responsive to MET-targeted therapies.

MATERIALS
Product Number
Brand
Product Description

Sigma-Aldrich
MISSION® shRNA Mouse Gene Family Set, DNA, Tyrosine Kinases
Sigma-Aldrich
MISSION® shRNA Mouse Gene Family Set, Lentiviral Particles, Tyrosine Kinases
Sigma-Aldrich
MISSION® shRNA Mouse Gene Family Set, Bacterial Glycerol Stock, Tyrosine Kinases