Uncoupling sodium channel dimers restores the phenotype of a pain-linked Nav 1.7 channel mutation.

Annika H RühlmannJannis KörnerRalf HausmannNikolay BebrivenskiChristian NeuhofSilvia Detro-DassenPetra HautvastCarène A BenasoloJannis E MeentsJan-Philipp MachtensGünther SchmalzingAngelika Lampert

Published in: British journal of pharmacology (2020)

Functional uncoupling of mutant hNav 1.7/A1632E channel dimers restored their defective allosteric fast inactivation mechanism. Our findings support the concept of sodium channel dimerization and reveal its potential relevance for human pain syndromes.

Keyphrases

chronic pain
pain management
neuropathic pain
endothelial cells
small molecule
nitric oxide synthase
genome wide
dna methylation
spinal cord injury
single cell
spinal cord
pluripotent stem cells
induced pluripotent stem cells