| Literature DB >> 25763473 |
Yong Liu1, Yunhui Lang1, Narendra Kumar Patel1, Grace Ng1, Radoslaw Laufer1, Sze-Wan Li1, Louise Edwards1, Bryan Forrest1, Peter B Sampson1, Miklos Feher1, Fuqiang Ban1, Donald E Awrey1, Irina Beletskaya1, Guodong Mao1, Richard Hodgson1, Olga Plotnikova1, Wei Qiu2, Nickolay Y Chirgadze2, Jacqueline M Mason1, Xin Wei1, Dan Chi-Chia Lin1, Yi Che1, Reza Kiarash1, Brian Madeira1, Graham C Fletcher1, Tak W Mak1, Mark R Bray1, Henry W Pauls1.
Abstract
The acetamido and carboxamido substituted 3-(1H-indazol-3-yl)benzenesulfonamides are potent TTK inhibitors. However, they display modest ability to attenuate cancer cell growth; their physicochemical properties, and attendant pharmacokinetic parameters, are not drug-like. By eliminating the polar 3-sulfonamide group and grafting a heterocycle at the 4 position of the phenyl ring, potent inhibitors with oral exposure were obtained. An X-ray cocrystal structure and a refined binding model allowed for a structure guided approach. Systematic optimization resulted in novel TTK inhibitors, namely 3-(4-(heterocyclyl)phenyl)-1H-indazole-5-carboxamides. Compounds incorporating the 3-hydroxy-8-azabicyclo[3.2.1]octan-8-yl bicyclic system were potent (TTK IC50 < 10 nM, HCT116 GI50 < 0.1 μM), displayed low off-target activity (>500×), and microsomal stability (T(1/2) > 30 min). A subset was tested in rodent PK and mouse xenograft models of human cancer. Compound 75 (CFI-401870) recapitulated the phenotype of TTK RNAi, demonstrated in vivo tumor growth inhibition upon oral dosing, and was selected for preclinical evaluation.Entities:
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Year: 2015 PMID: 25763473 DOI: 10.1021/jm501740a
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446