2-Aminopyridines as Potent and Selective Na v 1.8 Inhibitors Exhibiting Efficacy in a Nonhuman Primate Pain Model.
Michael J BreslinJeffrey W SchubertDeping WangChienjung HuangMichelle K ClementsYuxing LiXiaoping ZhouJoshua D VardiganRichard L KrausVincent P SantarelliJason M UslanerPaul J ColemanShawn J StachelPublished in: ACS medicinal chemistry letters (2024)
Herein we describe the discovery of a 2-aminopyridine scaffold as a potent and isoform selective inhibitor of the Na v 1.8 sodium channel. Parallel library synthesis, guided by in silico predictions, rapidly transformed initial hits into a novel 2-aminopyridine lead class possessing good ADME and pharmacokinetic profiles that were able to display activity in a clinically translatable nonhuman primate capsaicin-sensitized thermode pharmacodynamic assay. Progress toward the lead identification, optimization, and in vivo efficacy of these compounds will be discussed.