The voltage-gated sodium channel Scn8a is a genetic modifier of severe myoclonic epilepsy of infancy

doi:10.1093/hmg/ddm248

Human Molecular Genetics Advance Access originally published online on September 19, 2007
Human Molecular Genetics 2007 16(23):2892-2899; doi:10.1093/hmg/ddm248

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The voltage-gated sodium channel Scn8a is a genetic modifier of severe myoclonic epilepsy of infancy

Melinda S. Martin¹, Bin Tang¹, Ligia A. Papale², Frank H. Yu³, William A. Catterall³ and Andrew Escayg¹^,*

¹ Department of Human Genetics, Emory University, Atlanta, GA 30322, USA, ² Department of Psychobiology, Universidade Federal de São Paulo, São Paulo, Brazil and ³ Department of Pharmacology, University of Washington, Seattle, WA 98195, USA

^* To whom correspondence should be addressed at: Department of Human Genetics, Emory University, 615 Michael Street, Whitehead Building, Suite 301, Atlanta, GA 30322. Tel: +1 4047128328; Fax: +1 4047273949; Email: aescayg{at}genetics.emory.edu

Received July 5, 2007; Accepted August 23, 2007

The mammalian genome contains four voltage-gated sodium channelgenes that are primarily expressed in the central nervous system:SCN1A, SCN2A, SCN3A and SCN8A. Mutations in SCN1A and SCN2Aare responsible for several dominant idiopathic epilepsy disorders,including generalized epilepsy with febrile seizures plus (GEFS+)and severe myoclonic epilepsy of infancy (SMEI). Mutations inSCN8A are associated with cognitive deficits and neuropsychiatricillness in humans and movement disorders in mice; however, arole for SCN8A (Na_v1.6) in epilepsy has not been investigated.To determine the relationship between Na_v1.6 dysfunction andseizure susceptibility, we examined the thresholds of two Scn8amouse mutants, Scn8a^med and Scn8a^med-jo, to flurothyl- and kainicacid (KA)-induced seizures. Both mutants were more seizure resistantthan wild-type littermates, suggesting that altered Na_v1.6 functionreduces neuronal excitability. To determine whether impairedNa_v1.6 function could ameliorate seizure severity in a mousemodel of SMEI, we generated Scn1a^+/–; Scn8a^med-jo/+ doubleheterozygous mice. Unlike Scn1a^+/– mice that are moresusceptible to flurothyl-induced seizures, Scn1a^+/–; Scn8a^med-jo/+mice displayed thresholds that were comparable to wild-typelittermates. The Scn8a^med-jo allele was also able to rescuethe premature lethality of Scn1a^+/– mice and extend thelifespan of Scn1a^–/– mutants. These results demonstratethat genetic interactions can alter seizure severity and supportthe hypothesis that genetic modifiers contribute to the clinicalvariability observed in SMEI and GEFS+.

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