Synaptic dysregulation in a mouse model of GRIN2D developmental and epileptic encephalopathy.

Authors

JiaJie Teoh
Jane Simko
Chad R Camp
Christine J Liu
Wanqi Wang
Damian J Williams
Liang Ma
Divyalakshmi Soundararajan
Caryn Martin
Noah K Taylor
Ekniel François
Sabrina Petri
Ayla Kanber
Aishwarya Ravichandra
Maria Elena Pero
Francesca Bartolini
Theresa C Swayne
Cathleen Lutz, The Jackson LaboratoryFollow
Aamir Zuberi, The Jackson LaboratoryFollow
Moran Rubinstein
Moran Hausman-Kedem
Hongjie Yuan
Jennifer N Gelinas
Tristan T Sands
Scott Q Harper
Stephen F Traynelis
Christopher D Makinson
Wayne N Frankel

Document Type

Article

Publication Date

11-4-2025

Original Citation

Teoh J, Simko J, Camp C, Liu C, Wang W, Williams D, Ma L, Soundararajan D, Martin C, Taylor N, François E, Petri S, Kanber A, Ravichandra A, Pero M, Bartolini F, Swayne T, Lutz C, Zuberi A, Rubinstein M, Hausman-Kedem M, Yuan H, Gelinas J, Sands T, Harper S, Traynelis S, Makinson C, Frankel W. Synaptic dysregulation in a mouse model of GRIN2D developmental and epileptic encephalopathy. Brain. 2025;148(11):3973–88.

Keywords

Animals, Receptors, N-Methyl-D-Aspartate, Mice, Disease Models, Animal, Synapses, Epilepsy, Male, Gain of Function Mutation, Female, Hippocampus, Mice, Inbred C57BL

JAX Source

Brain. 2025;148(11):3973–88.

ISSN

1460-2156

PMID

40200555

DOI

https://doi.org/10.1093/brain/awaf125

Abstract

Gain-of-function (GoF) variants in the GRIN2D gene, encoding the GluN2D subunit of the N-methyl-D-aspartate receptor (NMDAR), cause a severe developmental and epileptic encephalopathy (DEE) characterized by intractable seizures, hypotonia and neurodevelopmental delay. We generated mice carrying the GoF V664I variant, orthologous to V667I, which is present in ∼25% of GRIN2D-DEE patients. Heterozygous mutant mice demonstrate behavioural, neuroanatomical and electrophysiological abnormalities. Lethal convulsive seizures are observed beginning at postnatal Day 17. As adults, heterozygotes display abundant and prolonged runs of spike-wave discharges (SWD) that often persist for minutes. The SWD epochs consist of different populations, differentiated by frequency and association with time-locked behavioural arrest. V664I mutant neurons have enlarged presynaptic terminals and increased synaptic distance. Functional analysis reveals increased inhibitory synaptic activity without changes in NMDAR decay kinetics or presynaptic plasticity in CA1 neurons, and analysis of hippocampal local field potentials shows a 1.5-fold increase in evoked responses and a 1.7-fold increase in action potential generation. Notably, expression of V664I in GABAergic interneurons, but not excitatory forebrain neurons, is sufficient to recapitulate the severe electroclinical phenotype. Altogether, our studies show that altered NMDAR function in inhibitory neurons plays a prominent role in DEE associated with GRIN2D GoF variants, suggesting that targeted genetic treatment may represent a path forward to successful therapeutic intervention.