| Literature DB >> 28512031 |
Jun Liang1, Sharada Labadie2, Birong Zhang2, Daniel F Ortwine2, Snahel Patel2, Maia Vinogradova2, James R Kiefer2, Till Mauer2, Victor S Gehling3, Jean-Christophe Harmange3, Richard Cummings3, Tommy Lai4, Jiangpeng Liao4, Xiaoping Zheng4, Yichin Liu2, Amy Gustafson2, Erica Van der Porten2, Weifeng Mao4, Bianca M Liederer2, Gauri Deshmukh2, Le An2, Yingqing Ran2, Marie Classon2, Patrick Trojer3, Peter S Dragovich2, Lesley Murray2.
Abstract
A high-throughput screening (HTS) of the Genentech/Roche library identified a novel, uncharged scaffold as a KDM5A inhibitor. Lacking insight into the binding mode, initial attempts to improve inhibitor potency failed to improve potency, and synthesis of analogs was further hampered by the presence of a C-C bond between the pyrrolidine and pyridine. Replacing this with a C-N bond significantly simplified synthesis, yielding pyrazole analog 35, of which we obtained a co-crystal structure with KDM5A. Using structure-based design approach, we identified 50 with improved biochemical, cell potency and reduced MW and lower lipophilicity (LogD) compared with the original hit. Furthermore, 50 showed lower clearance than 9 in mice. In combination with its remarkably low plasma protein binding (PPB) in mice (40%), oral dosing of 50 at 5mg/kg resulted in unbound Cmax ∼2-fold of its cell potency (PC9 H3K4Me3 0.96μM), meeting our criteria for an in vivo tool compound from a new scaffold.Entities:
Keywords: Epigenetics; KDM5; KDM5 inhibitors; Overcome cancer resistance; Structure-based drug discovery
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Year: 2017 PMID: 28512031 DOI: 10.1016/j.bmcl.2017.05.016
Source DB: PubMed Journal: Bioorg Med Chem Lett ISSN: 0960-894X Impact factor: 2.823