Molecules (Nov 2024)

Structure–Activity Relationship Studies in a Series of 2-Aryloxy-<i>N</i>-(pyrimidin-5-yl)acetamide Inhibitors of SLACK Potassium Channels

  • Nigam M. Mishra,
  • Brittany D. Spitznagel,
  • Yu Du,
  • Yasmeen K. Mohamed,
  • Ying Qin,
  • C. David Weaver,
  • Kyle A. Emmitte

DOI
https://doi.org/10.3390/molecules29235494
Journal volume & issue
Vol. 29, no. 23
p. 5494

Abstract

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Epilepsy of infancy with migrating focal seizures (EIMFS) is a rare, serious, and pharmacoresistant epileptic disorder often linked to gain-of-function mutations in the KCNT1 gene. KCNT1 encodes the sodium-activated potassium channel known as SLACK, making small molecule inhibitors of SLACK channels a compelling approach to the treatment of EIMFS and other epilepsies associated with KCNT1 mutations. In this manuscript, we describe a hit optimization effort executed within a series of 2-aryloxy-N-(pyrimidin-5-yl)acetamides that were identified via a high-throughput screen. We systematically prepared analogs in four distinct regions of the scaffold and evaluated their functional activity in a whole-cell, automated patch clamp (APC) assay to establish structure-activity relationships for wild-type (WT) SLACK inhibition. Two selected analogs were also profiled for selectivity versus other members of the Slo family of potassium channels, of which SLACK is a member, and versus a panel of structurally diverse ion channels. The same two analogs were evaluated for activity versus the WT mouse channel as well as two clinically relevant mutant human channels.

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