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2,4-Diaminopyrimidine MK2 inhibitors. Part I: Observation of an unexpected inhibitor binding mode
Authors:Maria A Argiriadi  Anna M Ericsson  Christopher M Harris  David L Banach  David W Borhani  David J Calderwood  Megan D Demers  Jennifer DiMauro  Richard W Dixon  Jennifer Hardman  Silvia Kwak  Biqin Li  John A Mankovich  Douglas Marcotte  Kelly D Mullen  Baofu Ni  M Pietras  Ramkrishna Sadhukhan  Silvino Sousa  Medha J Tomlinson  Robert V Talanian
Institution:Abbott Laboratories, 100 Research Drive, Worcester, MA 01605-5314, USA
Abstract:MK2 is a Ser/Thr kinase of significant interest as an anti-inflammatory drug discovery target. Here we describe the development of in vitro tools for the identification and characterization of MK2 inhibitors, including validation of inhibitor interactions with the crystallography construct and determination of the unique binding mode of 2,4-diaminopyrimidine inhibitors in the MK2 active site. Use of these tools in the optimization of a potent and selective inhibitor lead series is described in the accompanying Letter.
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