The developmental evolution of the seizure phenotype and cortical inhibition in mouse models of juvenile myoclonic epilepsy

Autor: Fazal Arain, Chengwen Zhou, Li Ding, Sahar Zaidi, Martin J. Gallagher
Jazyk: angličtina
Rok vydání: 2015
Předmět:
Zdroj: Neurobiology of Disease, Vol 82, Iss , Pp 164-175 (2015)
Druh dokumentu: article
ISSN: 1095-953X
DOI: 10.1016/j.nbd.2015.05.016
Popis: The GABAA receptor (GABAAR) α1 subunit mutation, A322D, causes autosomal dominant juvenile myoclonic epilepsy (JME). Previous in vitro studies demonstrated that A322D elicits α1(A322D) protein degradation and that the residual mutant protein causes a dominant-negative effect on wild type GABAARs. Here, we determined the effects of heterozygous A322D knockin (Hetα1AD) and deletion (Hetα1KO) on seizures, GABAAR expression, and motor cortex (M1) miniature inhibitory postsynaptic currents (mIPSCs) at two developmental time-points, P35 and P120. Both Hetα1AD and Hetα1KO mice experience absence seizures at P35 that persist at P120, but have substantially more frequent spontaneous and evoked polyspike wave discharges and myoclonic seizures at P120. Both mutant mice have increased total and synaptic α3 subunit expression at both time-points and decreased α1 subunit expression at P35, but not P120. There are proportional reductions in α3, β2, and γ2 subunit expression between P35 and P120 in wild type and mutant mice. In M1, mutants have decreased mIPSC peak amplitudes and prolonged decay constants compared with wild type, and the Hetα1AD mice have reduced mIPSC frequency and smaller amplitudes than Hetα1KO mice. Wild type and mutants exhibit proportional increases in mIPSC amplitudes between P35 and P120. We conclude that Hetα1KO and Hetα1AD mice model the JME subsyndrome, childhood absence epilepsy persisting and evolving into JME. Both mutants alter GABAAR composition and motor cortex physiology in a manner expected to increase neuronal synchrony and excitability to produce seizures. However, developmental changes in M1 GABAARs do not explain the worsened phenotype at P120 in mutant mice.
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