1区 · 医学
Article
作者: Aardalen, Kimberly ; Ramanathan, Anuradha ; Poddutoori, Ramulu ; Narayanan, Kishore ; Potakamuri, Ravi Kumar ; Gerken, Andrea ; Venetsanakos, Eleni ; Ramachandra, Murali ; Möbitz, Henrik ; Madapa, Sudharshan ; Perrone, Mark ; Pandit, Chetan ; Belliappa, Charamanna ; Subramanya, Hosahalli S. ; Aithal, Kiran ; Sager, Emine ; Krishnaswami, Maithreyi ; Gruenenfelder, Bjoern ; Samajdar, Susanta ; Chelur, Shekar ; Panigrahi, Sunil Kumar ; Barahagar, Sanjeev Surendranath ; Thimmasandra, Devaraja Seethappa ; Kiffe, Michael ; Langowski, John ; Gopinath, Sreevalsam ; Bock, Mark ; Ramos, Rita
Mutations in MEK1/2 have been described as a resistance mechanism to BRAF/MEK inhibitor treatment. We report the discovery of a novel ATP-competitive MEK1/2 inhibitor with efficacy in wildtype (WT) and mutant MEK12 models. Starting from a HTS hit, we obtained selective, cellularly active compounds that showed equipotent inhibition of WT MEK1/2 and a panel of MEK1/2 mutant cell lines. Using a structure-based approach, the optimization addressed the liabilities by systematic analysis of molecular matched pairs (MMPs) and ligand conformation. Addition of only three heavy atoms to early tool compound 6 removed Cyp3A4 liabilities and increased the cellular potency by 100-fold, while reducing log P by 5 units. Profiling of MAP855, compound 30, in pharmacokinetic-pharmacodynamic and efficacy studies in BRAF-mutant models showed comparable efficacy to clinical MEK1/2 inhibitors. Compound 30 is a novel highly potent and selective MEK1/2 kinase inhibitor with equipotent inhibition of WT and mutant MEK1/2, whose drug-like properties allow further investigation in the mutant MEK setting upon BRAF/MEK therapy.
