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Fragment-Based Discovery of 7-Azabenzimidazoles as Potent, Highly Selective, and Orally Active CDK4/6 Inhibitors

作者	CHO YOUNG SHIN; ANGOVE HAYLEY; BRAIN CHRISTOPHER; CHEN CHRISTINE HIUTUNG; CHENG HONG; CHENG ROBERT; CHOPRA RAJIV; CHUNG KRISTY; CONGREVE MILES; DAGOSTIN CLAUDIO; DAVIS DEBORAH J; FELTEN RUTH; GIRALDES JOHN; HISCOCK STEVEN D; KIM SUNKYU; KOVATS STEVEN; LAGU BHARAT; LEWRY KIM; LOO ALICE; LU YIPIN; LUZZIO MICHAEL; MANIARA WIESIA; MCMENAMIN RACHEL; MORTENSON PAUL N; BENNING RAJDEEP; OREILLY MARC; REES DAVID C; SHEN JUNQING; SMITH TROY; WANG YAPING; WILLIAMS GLYN; WOOLFORD ALISON J A; WRONA WOJCIECH; XU MEI; YANG FAN; HOWARD STEVEN

选自	期刊 ACS Medicinal Chemistry Letters; 卷期 2012年3-6; 页码 445-449

关联知识点

[摘要]：Herein, we describe the discovery of potent and highly selective inhibitors of both CDK4 and CDK6 via structure-guided optimization of a fragment-based screening hit. CDK6 X-ray crystallography and pharmacokinetic data steered efforts in identifying compound 6, which showed >1000-fold selectivity for CDK4 over CDKs 1 and 2 in an enzymatic assay. Furthermore, 6 demonstrated in vivo inhibition of pRb-phosphorylation and oral efficacy in a Jeko-1 mouse xenograft model.
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