Discovery of a potent CDK2 inhibitor with a novel binding mode, using virtual screening and initial, structure-guided lead scoping

Bioorg Med Chem Lett. 2007 Jul 15;17(14):3880-5. doi: 10.1016/j.bmcl.2007.04.110.

Christine M Richardson ¹, Claire L Nunns, Douglas S Williamson, Martin J Parratt, Pawel Dokurno, Rob Howes, Jenifer Borgognoni, Martin J Drysdale, Harry Finch, Roderick E Hubbard, Philip S Jackson, Peter Kierstan, Georg Lentzen, Jonathan D Moore, James B Murray, Heather Simmonite, Allan E Surgenor, Christopher J Torrance

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Affiliation

1 Vernalis (R&D) Ltd, Granta Park, Cambridge CB21 6GB, UK. [email protected]

PMID: 17570665 DOI: 10.1016/j.bmcl.2007.04.110

Abstract

Virtual screening against a pCDK2/cyclin A crystal structure led to the identification of a potent and novel CDK2 Inhibitor, which exhibited an unusual mode of interaction with the kinase binding motif. With the aid of X-ray crystallography and modelling, a medicinal chemistry strategy was implemented to probe the interactions seen in the crystal structure and to establish SAR. A fragment-based approach was also considered but a different, more conventional, binding mode was observed. Compound selectivity against GSK-3beta was improved using a rational design strategy, with crystallographic verification of the CDK2 binding mode.

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