| Literature DB >> 27490956 |
Paul Czodrowski1, Aurélie Mallinger2, Dirk Wienke1, Christina Esdar1, Oliver Pöschke1, Michael Busch1, Felix Rohdich1, Suzanne A Eccles2, Maria-Jesus Ortiz-Ruiz2, Richard Schneider1, Florence I Raynaud2, Paul A Clarke2, Djordje Musil1, Daniel Schwarz1, Trevor Dale3, Klaus Urbahns1, Julian Blagg2, Kai Schiemann1.
Abstract
The mediator complex-associated cyclin dependent kinase CDK8 regulates β-catenin-dependent transcription following activation of WNT signaling. Multiple lines of evidence suggest CDK8 may act as an oncogene in the development of colorectal cancer. Here we describe the successful optimization of an imidazo-thiadiazole series of CDK8 inhibitors that was identified in a high-throughput screening campaign and further progressed by structure-based design. In several optimization cycles, we improved the microsomal stability, potency, and kinase selectivity. The initial imidazo-thiadiazole scaffold was replaced by a 3-methyl-1H-pyrazolo[3,4-b]-pyridine which resulted in compound 25 (MSC2530818) that displayed excellent kinase selectivity, biochemical and cellular potency, microsomal stability, and is orally bioavailable. Furthermore, we demonstrated modulation of phospho-STAT1, a pharmacodynamic biomarker of CDK8 activity, and tumor growth inhibition in an APC mutant SW620 human colorectal carcinoma xenograft model after oral administration. Compound 25 demonstrated suitable potency and selectivity to progress into preclinical in vivo efficacy and safety studies.Entities:
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Year: 2016 PMID: 27490956 DOI: 10.1021/acs.jmedchem.6b00597
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446