Aminopyrazine Inhibitors Binding to an Unusual Inactive Conformation of the Mitotic Kinase Nek2: SAR and Structural Characterization

Daniel K Whelligan,Swen Hoelder,Corine Mas-Droux,Charles G Grummitt,Kwai-Ming J Cheung,Rob L M Van Montfort,G Wynne Aherne,Savade Solanki,Dawn Taylor,Samantha Burns,Caterina Barillari,Richard Bayliss,Douglas W Thomson,Kathy Boxall,Ian Collins

doi:10.1021/jm1008727

Daniel K Whelligan, Swen Hoelder + Show 13 more

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https://doi.org/10.1021/jm1008727

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Abstract

We report herein the first systematic exploration of inhibitors of the mitotic kinase Nek2. Starting from HTS hit aminopyrazine 2, compounds with improved activity were identified using structure-based design. Our structural biology investigations reveal two notable observations. First, 2 and related compounds bind to an unusual, inactive conformation of the kinase which to the best of our knowledge has not been reported for other types of kinase inhibitors. Second, a phenylalanine residue at the center of the ATP pocket strongly affects the ability of the inhibitor to bind to the protein. The implications of these observations are discussed, and the work described here defines key features for potent and selective Nek2 inhibition, which will aid the identification of more advanced inhibitors of Nek2.

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