Remarkable Phenytoin Sensitivity in 4 Children with SCN8A-related Epilepsy: A Molecular Neuropharmacological Approach

Publication date

2016-01-01

Authors

Boerma, Ragna S.
Braun, KeesISNI 0000000395904311
van den Broek, M P HISNI 0000000393141939
van Berkestijn, Frederique M CISNI 0000000393640754
Swinkels, Marielle E.ISNI 0000000394266717
Hagebeuk, Eveline O.
Lindhout, DickORCID 0000-0001-9580-624X
van Kempen, M J AISNI 0000000393375903
Boon, Maartje
Nicolai, Joost

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Abstract

Mutations in SCN8A are associated with epilepsy and intellectual disability. SCN8A encodes for sodium channel Nav1.6, which is located in the brain. Gain-of-function missense mutations in SCN8A are thought to lead to increased firing of excitatory neurons containing Nav1.6, and therefore to lead to increased seizure susceptibility. We hypothesized that sodium channel blockers could have a beneficial effect in patients with SCN8A-related epilepsy by blocking the overactive Nav1.6 and thereby counteracting the effect of the mutation. Herein, we describe 4 patients with a missense SCN8A mutation and epilepsy who all show a remarkably good response on high doses of phenytoin and loss of seizure control when phenytoin medication was reduced, while side effects were relatively mild. In 2 patients, repeated withdrawal of phenytoin led to the reoccurrence of seizures. Based on the findings in these patients and the underlying molecular mechanism we consider treatment with (high-dose) phenytoin as a possible treatment option in patients with difficult-to-control seizures due to an SCN8A mutation.

Keywords

epileptic encephalopathy, phenytoin, SCN8A, sodium channel blockers, Pharmacology (medical), Clinical Neurology, Pharmacology

Citation

Boerma, R S, Braun, K P, van den Broek, M P H, van Berkestijn, F M C, Swinkels, M E, Hagebeuk, E O, Lindhout, D, van Kempen, M, Boon, M, Nicolai, J, de Kovel, C G, Brilstra, E H & Koeleman, B P C 2016, 'Remarkable Phenytoin Sensitivity in 4 Children with SCN8A-related Epilepsy : A Molecular Neuropharmacological Approach', Neurotherapeutics , vol. 13, no. 1, pp. 192-197. https://doi.org/10.1007/s13311-015-0372-8