Structural Mechanisms Underlying Activation of TRPV1 Channels by Pungent Compounds in Gingers

Overview

Journal Br J Pharmacol

Publisher Wiley

Specialty Pharmacology

Date 2019 Jun 18

PMID 31207668

Citations 18

Authors

Yue Yin

Yawen Dong

Simon Vu

Fan Yang

Vladimir Yarov-Yarovoy

Yuhua Tian

Jie Zheng

Affiliations

Soon will be listed here.

Abstract

Background And Purpose: Like chili peppers, gingers produce pungent stimuli by a group of vanilloid compounds that activate the nociceptive transient receptor potential vanilloid 1 (TRPV1) ion channel. How these compounds interact with TRPV1 remains unclear.

Experimental Approach: We used computational structural modelling, functional tests (electrophysiology and calcium imaging), and mutagenesis to investigate the structural mechanisms underlying ligand-channel interactions.

Key Results: The potency of three principal pungent compounds from ginger -shogaol, gingerol, and zingerone-depends on the same two residues in the TRPV1 channel that form a hydrogen bond with the chili pepper pungent compound, capsaicin. Computational modelling revealed binding poses of these ginger compounds similar to those of capsaicin, including a "head-down tail-up" orientation, two specific hydrogen bonds, and important contributions of van der Waals interactions by the aliphatic tail. Our study also identified a novel horizontal binding pose of zingerone that allows it to directly interact with the channel pore when bound inside the ligand-binding pocket. These observations offer a molecular level explanation for how unique structures in the ginger compounds affect their channel activation potency.

Conclusions And Implications: Mechanistic insights into the interactions of ginger compounds and the TRPV1 cation channel should help guide drug discovery efforts to modulate nociception.

Citing Articles

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