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

Young Shin Cho,Hayley Angove,Christopher Thomas Brain,C. H. Chen,Hong Cheng,Robert Cheng,Rajiv Chopra,Kristy Chung,Miles Congreve,Claudio Dagostin,Deborah J. Davis,Ruth Feltell,John William Giraldes,S. Hiscock,Sunkyu Kim,Steven Kovats,Bharat Lagu,Kim Lewry,Alice Loo,Yipin Lu,Michael Luzzio,Wiesia Maniara,Rachel McMenamin,Paul N. Mortenson,Rajdeep Kaur Benning,Marc O’Reilly,David C. Rees,Junqing Shen,Troy Smith,Yaping Wang,Glyn Williams,Alison Jo-Anne Woolford,Wojciech Wrona,Mei Xu,Fan Yang,Steven Howard

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

2012

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.

Keywords:

Biochemistry
Cyclin-dependent kinase 6
Biology
Enzyme
Pharmacology
Cyclin-dependent kinase
Mantle cell lymphoma
In vivo
Pharmacokinetics
Transferase
orally active
highly selective

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