| Literature DB >> 31525968 |
Thilo Focken1, Kristen Burford1, Michael E Grimwood1, Alla Zenova1, Jean-Christophe Andrez1, Wei Gong1, Michael Wilson1, Matt Taron1, Shannon Decker1, Verner Lofstrand1, Sultan Chowdhury1, Noah Shuart1, Sophia Lin1, Samuel J Goodchild1, Clint Young1, Maegan Soriano1, Parisa K Tari1, Matthew Waldbrook1, Karen Nelkenbrecher1, Rainbow Kwan1, Andrea Lindgren1, Gina de Boer1, Stephanie Lee1, Luis Sojo1, Robert J DeVita2, Charles J Cohen1, Steven S Wesolowski1, J P Johnson1, Christoph M Dehnhardt1, James R Empfield1.
Abstract
Nonselective antagonists of voltage-gated sodium (NaV) channels have been long used for the treatment of epilepsies. The efficacy of these drugs is thought to be due to the block of sodium channels on excitatory neurons, primarily NaV1.6 and NaV1.2. However, these currently marketed drugs require high drug exposure and suffer from narrow therapeutic indices. Selective inhibition of NaV1.6, while sparing NaV1.1, is anticipated to provide a more effective and better tolerated treatment for epilepsies. In addition, block of NaV1.2 may complement the anticonvulsant activity of NaV1.6 inhibition. We discovered a novel series of aryl sulfonamides as CNS-penetrant, isoform-selective NaV1.6 inhibitors, which also displayed potent block of NaV1.2. Optimization focused on increasing selectivity over NaV1.1, improving metabolic stability, reducing active efflux, and addressing a pregnane X-receptor liability. We obtained compounds 30-32, which produced potent anticonvulsant activity in mouse seizure models, including a direct current maximal electroshock seizure assay.Entities:
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Year: 2019 PMID: 31525968 DOI: 10.1021/acs.jmedchem.9b01032
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446