Deciphering the role of epigenetics in self-limited epilepsy with centrotemporal spikes
Version 2 2024-06-04, 13:36Version 2 2024-06-04, 13:36
Version 1 2019-08-02, 08:07Version 1 2019-08-02, 08:07
journal contribution
posted on 2024-06-04, 13:36 authored by N Mohandas, YJ Loke, L Mackenzie, C Bennett, SF Berkovic, Jeffrey CraigJeffrey Craig, L Vadlamudi© 2019 Elsevier B.V. Objective: The aetiology of self-limited epilepsy with centro-temporal spikes (SECTS) remains controversial and a strong genetic basis has long been presumed. The discordant monozygotic twin (MZ) model controls for shared genetic and environmental factors, enabling focus on the potential role of the non-shared environment. Methods: DNA methylation data was acquired from DNA extracted from three discordant MZ twin pairs, from both new born blood spots before epilepsy onset, and blood samples taken after epilepsy onset. An epigenome-wide analysis was performed, using the Illumina Infinium EPIC array. Differentially methylated regions (DMR) were identified using the bumphunter package in R. Comparative analyses were undertaken at the two different time points as well as a combined analysis independent of time. Results: Many of the top DMR-associated genes have previously been described in neurodevelopmental disorders. The LYPD8 gene was associated with a top-ranked DMR both at birth and across the two time points. Conclusion: We have demonstrated the novel utility of the longitudinal, discordant MZ twin model, to facilitate a deeper appreciation of the complex neurobiology of SECTS. The genetic architecture of SECTS is complex and is likely to involve an interplay between genes and environment, in part mediated by epigenetics.
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Journal
Epilepsy ResearchVolume
156Article number
ARTN 106163Location
NetherlandsPublisher DOI
ISSN
0920-1211eISSN
1872-6844Language
EnglishPublication classification
C1 Refereed article in a scholarly journalCopyright notice
2019, Elsevier B.V.Publisher
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