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Literature DB >> 30190843

Oncogene-directed small molecule inhibitors for the treatment of cutaneous melanoma.

Philip Eliades^1,2,1,2, Keith T Flaherty^3,3, Hensin Tsao^1,1.

Abstract

Achievements in cancer genetics and molecular biology have revolutionized the treatment options available for advanced melanoma. Patients with certain molecularly defined melanomas have been the most fortunate beneficiaries of recently US FDA-approved therapies that target aberrant MAPK pathway signaling, yet response rates and duration of response remain suboptimal. Furthermore, many patients harbor melanomas for which no approved targeted therapies currently exist. Since the approval of vemurafenib, a selective BRAF V600E inhibitor, in 2011, there has been a surge of preclinical and clinical studies aimed at developing novel targeted therapies for a wide range of molecularly defined melanomas. In this review, we will examine the present status and future potential of molecularly targeted therapies directed at the most significant oncogenic signaling pathways in melanoma.

Entities: Chemical Disease Gene Mutation Species

Keywords: KIT; MAPK pathway; PI3K pathway; TCGA; melanoma; oncogene-directed therapy; small molecule inhibitor; targeted therapy

Year: 2015 PMID： 30190843 PMCID： PMC6094676 DOI： 10.2217/mmt.15.5

Source DB: PubMed Journal: Melanoma Manag ISSN： 2045-0885

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