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Expert Opinion on Investigational Drugs Volume 17, 2008 - Issue 7
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Review

Targeting the c-MET signaling pathway for cancer therapy

Xiangdong Liu Incyte Corporation, Experimental Station, Rt. 141 & Henry Clay Road, Wilmington, DE 19880, USA +1 302 498 6815; +1 302 425 2760; [email protected]
, PhD,
Wenqing Yao Incyte Corporation, Experimental Station, Rt. 141 & Henry Clay Road, Wilmington, DE 19880, USA +1 302 498 6815; +1 302 425 2760; [email protected]
, PhD,
Robert C Newton Incyte Corporation, Experimental Station, Rt. 141 & Henry Clay Road, Wilmington, DE 19880, USA +1 302 498 6815; +1 302 425 2760; [email protected]
, PhD &
Peggy A Scherle Incyte Corporation, Experimental Station, Rt. 141 & Henry Clay Road, Wilmington, DE 19880, USA +1 302 498 6815; +1 302 425 2760; [email protected]
, PhD
Pages 997-1011 | Published online: 12 Jun 2008
 
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Abstract

Background: In many human cancers, c-MET is activated via receptor overexpression, amplification, mutation and/or a ligand-dependent autocrine/paracrine loop. These biochemical and genetic abnormalities have been correlated with poor clinical outcomes and drug resistance in cancer patients. Preclinical studies suggest that targeting aberrant c-MET signaling could be an attractive therapy in cancer, but this notion has only recently been tested in the clinic. Objectives: To describe the biological aspects of the c-MET signaling pathway and to discuss recent progress and possible future trends in the development of agents that target the c-MET pathway, with an emphasis on small-molecule c-MET kinase inhibitors. Method: A review of relevant publications, including published articles in literature, reports at scientific meetings, and information available through the Internet. Results/conclusion: The dysregulated c-MET pathway represents a promising target for cancer drug development. The agents that target the c-MET pathway have demonstrated impressive evidence of early clinical activity and may have a significant therapeutic potential.

Notes

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