Reducing Agents Sensitize C-Type Nociceptors by Relieving High-Affinity Zinc Inhibition of T-Type Calcium Channels

Abstract

Recent studies have demonstrated an important role for T-type Ca²⁺channels (T-channels) in controlling the excitability of peripheral pain-sensing neurons (nociceptors). However, the molecular mechanisms underlying the functions of T-channels in nociceptors are poorly understood. Here, we demonstrate that reducing agents as well as endogenous metal chelators sensitize C-type dorsal root ganglion nociceptors by chelating Zn²⁺ions off specific extracellular histidine residues on Ca_v3.2 T-channels, thus relieving tonic channel inhibition, enhancing Ca_v3.2 currents, and lowering the threshold for nociceptor excitabilityin vitroandin vivo. Collectively, these findings describe a novel mechanism of nociceptor sensitization and firmly establish reducing agents, as well as Zn²⁺, Zn²⁺-chelating amino acids, and Zn²⁺-chelating proteins as endogenous modulators of Ca_v3.2 and nociceptor excitability.