Incidence of the V600K mutation among melanoma patients with BRAF mutations, and potential therapeutic response to the specific BRAF inhibitor PLX4032

Jill C. Rubinstein; Mario Sznol; Anna C. Pavlick; Stephan Ariyan; Elaine Cheng; Antonella Bacchiocchi; Harriet M. Kluger; Deepak Narayan; Ruth Halaban

doi:10.1186/1479-5876-8-67

Incidence of the V600K mutation among melanoma patients with BRAF mutations, and potential therapeutic response to the specific BRAF inhibitor PLX4032

Jill C. Rubinstein(Yale University), Mario Sznol(Yale University), Anna C. Pavlick(New York University), Stephan Ariyan(Yale University), Elaine Cheng(Yale University), Antonella Bacchiocchi(Yale University), Harriet M. Kluger(Yale University), Deepak Narayan(Yale University), Ruth Halaban(Yale University)

Journal of Translational Medicine

July 14, 2010

10.1186/1479-5876-8-67

Cited by 249Open Access

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Abstract

Activating mutations in BRAF kinase are common in melanomas. Clinical trials with PLX4032, the mutant-BRAF inhibitor, show promising preliminary results in patients selected for the presence of V600E mutation. However, activating V600K mutation is the other most common mutation, yet patients with this variant are currently excluded from the PLX4032 trials. Here we present evidence that a patient bearing the BRAF V600K mutation responded remarkably to PLX4032, suggesting that clinical trials should include all patients with activating BRAF V600E/K mutations.

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