| Literature DB >> 21916012 |
Craig A Coburn1, Yunfu Luo, Mingxiang Cui, Jiabing Wang, Richard Soll, Jingchao Dong, Bin Hu, Michael A Lyon, Vincent P Santarelli, Richard L Kraus, Yun Gregan, Yi Wang, Steven V Fox, Jacquelyn Binns, Scott M Doran, Duane R Reiss, Pamela L Tannenbaum, Anthony L Gotter, Peter T Meinke, John J Renger.
Abstract
TWIK-related acid-sensitive K(+) (K(2P) 9.1, TASK-3) ion channels have the capacity to regulate the activity of neuronal pathways by influencing the resting membrane potential of neurons on which they are expressed. The central nervous system (CNS) expression of these channels suggests potential roles in neurologic disorders, and it is believed that the development of TASK-3 antagonists could lead to the therapeutic treatment of a number of neurological conditions. While a therapeutic potential for TASK-3 channel modulation exists, there are only a few documented examples of potent and selective small-molecule channel blockers. Herein, we describe the discovery and lead optimization efforts for a novel series of TASK-3 channel antagonists based on a 5,6,7,8-tetrahydropyrido[4,3-d]pyrimidine high-throughput screening lead from which a subseries of potent and selective inhibitors were identified. One compound was profiled in detail with respect to its physical properties and demonstrated pharmacological target engagement as indicated by its ability to modulate sleep architecture in rodent electroencephalogram (EEG) telemetry models.Entities:
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Year: 2011 PMID: 21916012 DOI: 10.1002/cmdc.201100351
Source DB: PubMed Journal: ChemMedChem ISSN: 1860-7179 Impact factor: 3.466