Optimized 4,5-Diarylimidazoles as Potent/Selective Inhibitors of Protein Kinase CK1 delta and Their Structural Relation to p38 alpha MAPK.
Halekotte, J., Witt, L., Ianes, C., Kruger, M., Buhrmann, M., Rauh, D., Pichlo, C., Brunstein, E., Luxenburger, A., Baumann, U., Knippschild, U., Bischof, J., Peifer, C.(2017) Molecules 22
- PubMed: 28338621 
- DOI: https://doi.org/10.3390/molecules22040522
- Primary Citation of Related Structures:  
5ML5, 5MQV - PubMed Abstract: 
The involvement of protein kinase CK1¦Ä in the pathogenesis of severe disorders such as Alzheimer's disease, amyotrophic lateral sclerosis, familial advanced sleep phase syndrome, and cancer has dramatically increased interest in the development of effective small molecule inhibitors for both therapeutic application and basic research. Unfortunately, the design of CK1 isoform-specific compounds has proved to be highly complicated due to the existence of six evolutionarily conserved human CK1 members that possess similar, different, or even opposite physiological and pathophysiological implications. Consequently, only few potent and selective CK1¦Ä inhibitors have been reported so far and structurally divergent approaches are urgently needed in order to establish SAR that might enable complete discrimination of CK1 isoforms and related p38¦Á MAPK. In this study we report on design and characterization of optimized 4,5-diarylimidazoles as highly effective ATP-competitive inhibitors of CK1¦Ä with compounds 11b (IC 50 CK1¦Ä = 4 nM, IC 50 CK1¦Å = 25 nM), 12a (IC 50 CK1¦Ä = 19 nM, IC 50 CK1¦Å = 227 nM), and 16b (IC 50 CK1¦Ä = 8 nM, IC 50 CK1¦Å = 81 nM) being among the most potent CK1¦Ä-targeting agents published to date. Inhibitor compound 11b , displaying potential as a pharmacological tool, has further been profiled over a panel of 321 protein kinases exhibiting high selectivity. Cellular efficacy has been evaluated in human pancreatic cancer cell lines Colo357 (EC 50 = 3.5 ?M) and Panc89 (EC 50 = 1.5 ?M). SAR is substantiated by X-ray crystallographic analysis of 16b in CK1¦Ä and 11b in p38¦Á.
Organizational Affiliation: 
Institute of Pharmacy, Christian-Albrechts-University of Kiel, Gutenbergstra?e 76, D-24118 Kiel, Germany. jhalekotte@pharmazie.uni-kiel.de.