| Literature DB >> 34055223 |
V Blair Journigan1,2, David Alarcón-Alarcón3, Zhiwei Feng4,5,6, Yuanqiang Wang4,5,6, Tianjian Liang4,5,6, Denise C Dawley1, A R M Ruhul Amin1,2, Camila Montano7,8,9, Wade D Van Horn7,8,9, Xiang-Qun Xie4,5,6, Antonio Ferrer-Montiel3, Asia Fernández-Carvajal3.
Abstract
TRPM8 antagonists derived from its cognate ligand, (-)-menthol, are underrepresented. We determine the absolute stereochemistry of a well-known TRPM8 antagonist, (-)-menthyl 1, using VCD and 2D NMR. We explore 1 for its antagonist effects of the human TRPM8 (hTRPM8) orthologue to uncover species-dependent inhibition versus rat channels. (-)-Menthyl 1 inhibits menthol- and icilin-evoked Ca2+ responses at hTRPM8 with IC50 values of 805 ± 200 nM and 1.8 ± 0.6 μM, respectively, while more potently inhibiting agonist responses at the rat orthologue (rTRPM8 IC50 (menthol) = 117 ± 18 nM, IC50 (icilin) = 521 ± 20 nM). Whole-cell patch-clamp recordings of hTRPM8 confirm the 1 inhibition of menthol-stimulated currents, with an IC50 of 700 ± 200 nM. We demonstrate that 1 possesses ≥400-fold selectivity for hTRPM8 versus hTRPA1/hTRPV1. (-)-menthyl 1 can be used as a novel chemical tool to study hTRPM8 pharmacology and differences in species commonly used in drug discovery.Entities:
Year: 2021 PMID: 34055223 PMCID: PMC8155240 DOI: 10.1021/acsmedchemlett.1c00001
Source DB: PubMed Journal: ACS Med Chem Lett ISSN: 1948-5875 Impact factor: 4.345