Mutations associated with epileptic encephalopathy modify EAAT2 anion channel function.

Peter Kovermann Yulia KolobkovaArne FranzenChristoph Fahlke

Published in: Epilepsia (2021)

l-glutamate permeability of the EAAT anion pore is an unexpected functional consequence of naturally occurring single amino acid substitutions. l-glutamate efflux through mutant EAAT2 anion channels will cause glutamate excitotoxicity and neuronal hyperexcitability in affected patients. Antagonists that selectively suppress the EAAT anion channel function could serve as therapeutic agents in the future.

Keyphrases

ionic liquid
amino acid
end stage renal disease
ejection fraction
newly diagnosed
endothelial cells
early onset
patient reported outcomes
current status
brain injury
subarachnoid hemorrhage
wild type