| Literature DB >> 35671848 |
Ciria C Hernandez1, Rahilla A Tarfa2, Jose Miguel I Limcaoco3, Ruiting Liu4, Pravat Mondal4, Clare Hill5, R Keith Duncan6, Thanos Tzounopoulos2, Corey R J Stephenson7, Matthew J O'Meara3, Peter Wipf8.
Abstract
To identify pore domain ligands on Kv7.2 potassium ion channels, we compared wild-type (WT) and W236L mutant Kv7.2 channels in a series of assays with previously validated and novel agonist chemotypes. Positive controls were retigabine, flupirtine, and RL-81; i.e. Kv7.2 channel activators that significantly shift voltage-dependent activation to more negative potentials (ΔV50) at 5 µM. We identified 6 new compounds that exhibited differential enhancing activity between WT and W236L mutant channels. Whole cell patch-clamp electrophysiology studies were conducted to identify Kv7.2. Kv7.2/3, Kv7.4, and Kv7.5 selectivity. Our results validate the SyncroPatch platform and establish new structure activity relationships (SAR). Specifically, in addition to selective Kv7.2, Kv7.2/3, Kv7.4. and Kv7.5 agonists, we identified a novel chemotype, ZK-21, a 4-aminotetrahydroquinoline that is distinct from any of the previously described Kv7 channel modifiers. Using flexible receptor docking, ZK-21 was predicted to be stabilized by W236 and bind perpendicular to retigabine, burying the benzyl carbamate group into a tunnel reaching the core of the pore domain.Entities:
Keywords: Agonists; Potassium channels; Quinolines; SyncroPatch screen; Voltage-dependent activation
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Year: 2022 PMID: 35671848 PMCID: PMC9469649 DOI: 10.1016/j.bmcl.2022.128841
Source DB: PubMed Journal: Bioorg Med Chem Lett ISSN: 0960-894X Impact factor: 2.940