Hippocampal hyperexcitability and specific epileptiform activity in a mouse model of D ravet syndrome

C Liautard, P Scalmani, G Carriero, M de Curtis… - …, 2013 - Wiley Online Library
C Liautard, P Scalmani, G Carriero, M de Curtis, S Franceschetti, M Mantegazza
Epilepsia, 2013Wiley Online Library
Purpose D ravet syndrome (DS) is caused by dominant mutations of the SCN1A gene,
encoding the N aV1. 1 sodium channel α subunit. Gene targeted mouse models of DS
mutations replicate patients' phenotype and show reduced γ‐aminobutyric acid (GABA)
ergic inhibition. However, little is known on the properties of network hyperexcitability and on
properties of seizure generation in these models. In fact, seizures have been studied thus far
with surface electroencephalography (EEG), which did not show if specific brain regions are …
Purpose
Dravet syndrome (DS) is caused by dominant mutations of the SCN1A gene, encoding the NaV1.1 sodium channel α subunit. Gene targeted mouse models of DS mutations replicate patients' phenotype and show reduced γ‐aminobutyric acid (GABA)ergic inhibition. However, little is known on the properties of network hyperexcitability and on properties of seizure generation in these models. In fact, seizures have been studied thus far with surface electroencephalography (EEG), which did not show if specific brain regions are particularly involved. We have investigated hyperexcitability and epileptiform activities generated in neuronal networks of a mouse model of DS.
Methods
We have studied heterozygous NaV1.1 knock‐out mice performing field potential recordings in combined hippocampal/cortical slices in vitro and video/depth electrode intracerebral recordings in vivo during hyperthermia‐induced seizures.
Key Findings
In slices, we have disclosed specific signs of hyperexcitability of hippocampal circuits in both the pre‐epileptic and epileptic periods, and a specific epileptiform activity was generated in the hippocampus upon application of the convulsant 4‐aminopyridine in the epileptic period. During in vivo hyperthermia‐induced seizures, we have observed selective hippocampal activity in early preictal phases and pronounced hippocampal activity in the ictal phase.
Significance
We have identified specific epileptiform activities and signs of network hyperexcitability, and disclosed the important role of the hippocampus in seizure generation in this model. These activities may be potentially used as targets for screenings of antiepileptic approaches.
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