Sodium valproate is associated with cortical thinning of disease-specific areas in juvenile myoclonic epilepsy

Author:

Crespo Pimentel BernardoORCID,Kuchukhidze Giorgi,Xiao FenglaiORCID,Caciagli Lorenzo,Höfler Julia,Rainer Lucas,Kronbichler Martin,Vollmar Christian,Duncan John SORCID,Trinka Eugen,Koepp Matthias,Wandschneider Britta

Abstract

BackgroundJuvenile myoclonic epilepsy (JME) is associated with cortical thinning of the motor areas. The relative contribution of antiseizure medication to cortical thickness is unknown. We aimed to investigate how valproate influences the cortical morphology of JME.MethodsIn this cross-sectional study, individuals with JME with and without valproate, with temporal lobe epilepsy (TLE) with valproate and controls were selected through propensity score matching. Participants underwent T1-weighted brain imaging and vertex-wise calculation of cortical thickness.ResultsWe matched 36 individuals with JME on valproate with 36 individuals with JME without valproate, 36 controls and 19 individuals with TLE on valproate. JME on valproate showed thinning of the precentral gyri (left and right, p<0.001) compared with controls and thinning of the left precentral gyrus when compared with JME not on valproate (p<0.01) or to TLE on valproate (p<0.001). Valproate dose correlated negatively with the thickness of the precentral gyri, postcentral gyri and superior frontal gyrus in JME (left and right p<0.0001), but not in TLE.ConclusionsValproate was associated with JME-specific and dose-dependent thinning of the cortical motor regions. This suggests that valproate is a key modulator of cortical morphology in JME, an effect that may underlie its high efficacy in this syndrome.

Funder

Austrian Science Fund

Henry Smith Charity

Wellcome Trust

Publisher

BMJ

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