Myoclonic status epilepticus and cerebellar hypoplasia associated with a novel variant in the GRIA3 gene

Berardo Rinaldi,Cristina Gervasini,Elena Freri,Arianna Tucci,Jia-Hui Sun,Donatella Milani,Henry Houlden,Margherita Estienne,Tiziana Granata,Allan Bayat,Stephanie Efthymiou,Bénédicte Gérard,Yu-Han Ge,Paola Marchisio,Yun Stone Shi

doi:10.1007/s10048-021-00666-1

Abstract

AMPA-type glutamate receptors (AMPARs) are postsynaptic ionotropic receptors which mediate fast excitatory currents. AMPARs have a heterotetrameric structure, variably composed by the four subunits GluA1-4 which are encoded by genes GRIA1-4. Increasing evidence support the role of pathogenic variants in GRIA1-4 genes as causative for syndromic intellectual disability (ID). We report an Italian pedigree where some male individuals share ID, seizures and facial dysmorphisms. The index subject was referred for severe ID, myoclonic seizures, cerebellar signs and short stature. Whole exome sequencing identified a novel variant in GRIA3, c.2360A > G, p.(Glu787Gly). The GRIA3 gene maps to chromosome Xq25 and the c.2360A > G variant was transmitted by his healthy mother. Subsequent analysis in the family showed a segregation pattern compatible with the causative role of this variant, further supported by preliminary functional insights. We provide a detailed description of the clinical evolution of the index subjects and stress the relevance of myoclonic seizures and cerebellar syndrome as cardinal features of his presentation.

Highlights

The GRIA3 gene is located at Xq25 and encodes the AMPAtype glutamate receptor (AMPAR) subunit 3
Neurodevelopmental disorders (NDD) and epilepsy often coexist in individuals referred for genetic investigations
Few recent studies identified causative variants in genes encoding AMPAR subunits for individuals with NDD associated with epilepsy [15,16,17, 19, 24, 25]

Summary

Introduction

The GRIA3 gene is located at Xq25 and encodes the AMPAtype glutamate receptor (AMPAR) subunit 3. All the AMPAR genes express in vivo two different isoforms, generated by means of alternative splicing of exon 14 (flip/flop isoforms), which provides different kinetic behaviours and contributes to the functional richness of AMPARs [3, 6]. This tight regulation contributes to learning and memory processes via the synaptic plasticity [7,8,9]

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