Litcius/Paper detail

A plant‐derived TRPV3 inhibitor suppresses pain and itch

Yalan Han, Anna Luo, Peter Muiruri Kamau, Pitchayakarn Takomthong, Jingmei Hu, Chantana Boonyarat, Lei Luo, Ren Lai

2021British Journal of Pharmacology55 citationsDOIOpen Access PDF

Abstract

BACKGROUND AND PURPOSE: Itching is the most frequent pathology in dermatology that has significant impacts on people's mental health and social life. Transient receptor potential vanilloid 3 (TRPV3) channel is a promising target for treating pruritus. However, few selecetive and potent antagonists have been reported. This study was designed to identify selective TRPV3 antagonist and elucidate its anti-pruritus pharmacology. EXPERIMENTAL APPROACH: FlexStation and calcium fluorescence imaging were conducted to track the functional compounds. Whole-cell patch clamp was used to record itch-related ion channel currents. Homologous recombination and site-directed mutagenesis were employed to construct TRPV3 channel chimeras and point mutations for exploring pharmacological mechanism. Mouse models were used for in vivo anti-pruritus assay. KEY RESULTS: ) of 12.43 μM. Citrusinine-II showed potential efficacy to attenuate both chronic and acute itch. Intradermal administration of citrusinine-II (143 ng/skin site) nearly completely inhibited itch behaviours. It also shows significant analgesic effects. Little side effects of the compound are observed. CONCLUSION AND IMPLICATIONS: By acting as a selective and potent inhibitor of TRPV3 channel, citrusinine-II shows valuable therapeutic effects in pruritus animal models and is a promising candidate drug and/or lead molecule for the development of anti-pruritus drugs.

Topics & Concepts

PharmacologyTransient receptor potential channelMedicineItchingAntagonistAnalgesicIn vivoReceptorBiologyImmunologyInternal medicineBiotechnologyDermatology and Skin DiseasesIon Channels and ReceptorsHerbal Medicine Research Studies