Inhibition of the Human Neuronal Sodium Channel Nav1.9 by Arachidonyl-2-Chloroethylamide, An Analogue of Anandamide in a hNav1.9/rNav1.4 Chimera, An Experimental and in Silico Study

•hNav1.9_C4 chimera in CHOK-1 cells encompasses the extracellular and transmembrane domain of hNav1.9.•Synthetic cannabinoid ACEA blocked hNav1.9_C4+ß1 currents causing a hyperpolarizing shift in inactivation.•hNav1.9_C4 channels display window currents, significantly reduced by ACEA.•Computationall...

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Published in:Neuroscience 2023-02, Vol.511, p.39-52
Main Authors: Marchese-Rojas, Mario, Islas, Ángel A., Mancilla-Simbro, Claudia, Millan-PerezPeña, Lourdes, León, Jorge S., Salinas-Stefanon, Eduardo M.
Format: Article
Language:English
Subjects:
ACEA
AEA
analgesia
anandamide
cannabinoid
CHOK-1
docking
electrostatic complementarity
endocannabinoid
induced fit
LABS
local anestetics
Monte Carlo
Nav1.9
nociception
pain
patch clamp
sodium channel
window current
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Summary:•hNav1.9_C4 chimera in CHOK-1 cells encompasses the extracellular and transmembrane domain of hNav1.9.•Synthetic cannabinoid ACEA blocked hNav1.9_C4+ß1 currents causing a hyperpolarizing shift in inactivation.•hNav1.9_C4 channels display window currents, significantly reduced by ACEA.•Computationally, ACEA binds the local anaesthetic binding site.•The local anaesthetic profile of ACEA may be involved in cannabinoid analgesia. Cannabinoids regulate analgesia, which has aroused much interest in identifying new pharmacological therapies in the management of refractory pain. Voltage-gated Na+ channels (Navs) play an important role in inflammatory and neuropathic pain. In particular, Nav1.9 is involved in nociception and the understanding of its pharmacology has lagged behind because it is difficult to express in heterologous systems. Here, we utilized the chimeric channel hNav1.9_C4, that comprises the extracellular and transmembrane domains of hNav1.9, co-expressed with the ß1 subunit on CHO-K1 cells to characterize the electrophysiological effects of ACEA, a synthetic surrogate of the endogenous cannabinoid anandamide. ACEA induced a tonic block, decelerated the fast inactivation, markedly shifted steady-state inactivation in the hyperpolarized direction, decreasing the window current and showed use-dependent block, with a high affinity for the inactivated state (ki = 0.84 µM). Thus, we argue that ACEA possess a local anaesthetic-like profile. To provide a mechanistic understanding of its mode of action at the molecular level, we combined induced fit docking with Monte Carlo simulations and electrostatic complementarity. In agreement with the experimental evidence, our computer simulations revealed that ACEA binds Tyr1599 of the local anaesthetics binding site of the hNav1.9, contacting residues that bind cannabinol (CBD) in the NavMs channel. ACEA adopted a conformation remarkably similar to the crystallographic conformation of anandamide on a non-homologous protein, obstructing the Na+ permeation pathway below the selectivity filter to occupy a highly conserved binding pocket at the intracellular side. These results describe a mechanism of action, possibly involved in cannabinoid analgesia.
ISSN:0306-4522
1873-7544
DOI:10.1016/j.neuroscience.2022.09.015