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Discovery and Optimization of C-2 Methyl Imidazopyrrolopyridines as Potent and Orally Bioavailable JAK1 Inhibitors with Selectivity over JAK2

作者	ZAK MARK; MENDONCA ROHAN; BALAZS MERCEDESZ; BARRETT KATHY; BERGERON PHILIPPE; BLAIR WADE S; CHANG CHRISTINE; DESHMUKH GAURI; DEVOSS JASON; DRAGOVICH PETER S; EIGENBROT CHARLES; GHILARDI NICO; GIBBONS PAUL; GRADL STEFAN; HAMMAN CHRIS; HANAN EMILY J; HARSTAD ERIC; HEWITT PETER R; HURLEY CHRISTOPHER A; JIN TIAN; JOHNSON ADAM; JOHNSON TONY; KENNY JANE R; KOEHLER MICHAEL F T; KOHLI PAWAN BIR; KULAGOWSKI JANUSZ J; LABADIE SHARADA; LIAO JIANGPENG; LIIMATTA MARYA; LIN ZHONGHUA; LUPARDUS PATRICK J; MAXEY ROBERT J; MURRAY JEREMY M; PULK REBECCA; RODRIGUEZ MADELEINE; SAVAGE SCOTT; SHIA STEVEN; STEFFEK MICAH; UBHAYAKAR SAVITA; ULTSCH MARK; VAN ABBEMA ANNE; WARD STUART I; XIAO LING; XIAO YISONG

选自	期刊 Journal of Medicinal Chemistry; 卷期 2012年55-13; 页码 6176-6193

关联知识点

[摘要]：Herein we report the discovery of the C-2 methyl substituted imidazopyrrolopyridine series and its optimization to provide potent and orally bioavailable JAK1 inhibitors with selectivity over JAK2. The C-2 methyl substituted inhibitor 4 exhibited not only improved JAK1 potency relative to unsubstituted compound 3 but also notable JAK1 vs JAK2 selectivity (20-fold and >33-fold in biochemical and cell-based assays, respectively). Features of the X-ray structures of 4 in complex with both JAK1 and JAK2 are delineated. Efforts to improve the in vitro and in vivo ADME properties of 4 while maintaining JAK1 selectivity are described, culminating in the discovery of a highly optimized and balanced inhibitor (20). Details of the biological characterization of 20 are disclosed including JAK1 vs JAK2 selectivity levels, preclinical in vivo PK profiles, performance in an in vivo JAK1-mediated PK/PD model, and attributes of an X-ray structure in complex with JAK1.
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