Chemistry & Biology
Volume 17, Issue 10, 29 October 2010, Pages 1111-1121
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Article
Discovery and Characterization of 2-Anilino-4- (Thiazol-5-yl)Pyrimidine Transcriptional CDK Inhibitors as Anticancer Agents

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Summary

The main difficulty in the development of ATP antagonist kinase inhibitors is target specificity, since the ATP-binding motif is present in many proteins. We introduce a strategy that has allowed us to identify compounds from a kinase inhibitor library that block the cyclin-dependent kinases responsible for regulating transcription, i.e., CDK7 and especially CDK9. The screening cascade employs cellular phenotypic assays based on mitotic index and nuclear p53 protein accumulation. This permitted us to classify compounds into transcriptional, cell cycle, and mitotic inhibitor groups. We describe the characterization of the transcriptional inhibitor class in terms of kinase inhibition profile, cellular mode of action, and selectivity for transformed cells. A structural selectivity rationale was used to optimize potency and biopharmaceutical properties and led to the development of a transcriptional inhibitor, 3,4-dimethyl-5-[2-(4-piperazin-1-yl-phenylamino)-pyrimidin-4-yl]-3H-thiazol-2-one, with anticancer activity in animal models.

Highlights

► Phenotypic screening cascade to classify small-molecule kinase inhibitor compounds ► Three types of kinase inhibitors: transcriptional, mitotic, and cell cycle ► Structure-based design of CDK9-selective kinase inhibitor compounds ► A drug-like CDK9 inhibitor compound with in vivo activity

Cited by (0)

2

Present address: School of Pharmacy and Centre for Biomolecular Sciences, University of Nottingham, Nottingham NG7 2RD, UK

3

Present address: Veterinary School, University of Thessaly, Karditsa 43100, Greece

4

Present address: South Carolina College of Pharmacy, University of South Carolina, Columbia, SC 29208, USA