Title of article :
Discovery of a potent CDK2 inhibitor with a novel binding mode, using virtual screening and initial, structure-guided lead scoping
Author/Authors :
Christine M. Richardson، نويسنده , , Claire L. Nunns، نويسنده , , Douglas S. Williamson، نويسنده , , Martin J. Parratt، نويسنده , , Pawel Dokurno، نويسنده , , Rob Howes، نويسنده , , Jenifer Borgognoni، نويسنده , , Martin J. Drysdale، نويسنده , , Harry Finch، نويسنده , , Roderick E. Hubbard، نويسنده , , Philip S. Jackson، نويسنده , , Peter Kierstan، نويسنده , , Georg Lentzen، نويسنده , , Jonathan D. Moore، نويسنده , , James B. Murray، نويسنده , , Heather Simmonite، نويسنده , , Allan E. Surgenor، نويسنده , , Christopher J. Torrance، نويسنده ,
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-3β was improved using a rational design strategy, with crystallographic verification of the CDK2 binding mode.
Keywords :
Structure-guided drug design , Fragment based , Docking , Cyclin dependent kinase , CDK2 , X-ray crystallography , Virtual screening
