| Literature DB >> 25965804 |
James R Henry1, Michael D Kaufman2, Sheng-Bin Peng1, Yu Mi Ahn2, Timothy M Caldwell2, Lakshminarayana Vogeti2, Hanumaiah Telikepalli2, Wei-Ping Lu2, Molly M Hood2, Thomas J Rutkoski2, Bryan D Smith2, Subha Vogeti2, David Miller2, Scott C Wise2, Lawrence Chun3, Xiaoyi Zhang1, Youyan Zhang1, Lisa Kays1, Philip A Hipskind1, Aaron D Wrobleski1, Karen L Lobb1, Julia M Clay1, Jeffrey D Cohen1, Jennie L Walgren1, Denis McCann1, Phenil Patel1, David K Clawson1, Sherry Guo1, Danalyn Manglicmot1, Chris Groshong1, Cheyenne Logan1, James J Starling1, Daniel L Flynn2.
Abstract
The RAS-RAF-MEK-MAPK cascade is an essential signaling pathway, with activation typically mediated through cell surface receptors. The kinase inhibitors vemurafenib and dabrafenib, which target oncogenic BRAF V600E, have shown significant clinical efficacy in melanoma patients harboring this mutation. Because of paradoxical pathway activation, both agents were demonstrated to promote growth and metastasis of tumor cells with RAS mutations in preclinical models and are contraindicated for treatment of cancer patients with BRAF WT background, including patients with KRAS or NRAS mutations. In order to eliminate the issues associated with paradoxical MAPK pathway activation and to provide therapeutic benefit to patients with RAS mutant cancers, we sought to identify a compound not only active against BRAF V600E but also wild type BRAF and CRAF. On the basis of its superior in vitro and in vivo profile, compound 13 was selected for further development and is currently being evaluated in phase I clinical studies.Entities:
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Year: 2015 PMID: 25965804 DOI: 10.1021/acs.jmedchem.5b00067
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446