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Pyridyl aminothiazoles as potent inhibitors of Chk1 with slow dissociation rates
Authors:Dudkin Vadim Y  Rickert Keith  Kreatsoulas Constantine  Wang Cheng  Arrington Kenneth L  Fraley Mark E  Hartman George D  Yan Yowei  Ikuta Mari  Stirdivant Steven M  Drakas Robert A  Walsh Eileen S  Hamilton Kelly  Buser Carolyn A  Lobell Robert B  Sepp-Lorenzino Laura
Institution:Department of Medicinal Chemistry, Merck Research Laboratories, West Point, PA 19486, USA. vadim_dudkin@merck.com
Abstract:Pyridyl aminothiazoles comprise a novel class of ATP-competitive Chk1 inhibitors with excellent inhibitory potential. Modification of the core with ethylenediamine amides provides compounds with low picomolar potency and very high residence times. Investigation of binding parameters of such compounds using X-ray crystallography and molecular dynamics simulations revealed multiple hydrogen bonds to the enzyme backbone as well as stabilization of the conserved water molecules network in the hydrophobic binding region.
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