PLoS ONE (Jan 2018)

Rare gene deletions in genetic generalized and Rolandic epilepsies.

  • Kamel Jabbari,
  • Dheeraj R Bobbili,
  • Dennis Lal,
  • Eva M Reinthaler,
  • Julian Schubert,
  • Stefan Wolking,
  • Vishal Sinha,
  • Susanne Motameny,
  • Holger Thiele,
  • Amit Kawalia,
  • Janine Altmüller,
  • Mohammad Reza Toliat,
  • Robert Kraaij,
  • Jeroen van Rooij,
  • André G Uitterlinden,
  • M Arfan Ikram,
  • EuroEPINOMICS CoGIE Consortium,
  • Federico Zara,
  • Anna-Elina Lehesjoki,
  • Roland Krause,
  • Fritz Zimprich,
  • Thomas Sander,
  • Bernd A Neubauer,
  • Patrick May,
  • Holger Lerche,
  • Peter Nürnberg

DOI
https://doi.org/10.1371/journal.pone.0202022
Journal volume & issue
Vol. 13, no. 8
p. e0202022

Abstract

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Genetic Generalized Epilepsy (GGE) and benign epilepsy with centro-temporal spikes or Rolandic Epilepsy (RE) are common forms of genetic epilepsies. Rare copy number variants have been recognized as important risk factors in brain disorders. We performed a systematic survey of rare deletions affecting protein-coding genes derived from exome data of patients with common forms of genetic epilepsies. We analysed exomes from 390 European patients (196 GGE and 194 RE) and 572 population controls to identify low-frequency genic deletions. We found that 75 (32 GGE and 43 RE) patients out of 390, i.e. ~19%, carried rare genic deletions. In particular, large deletions (>400 kb) represent a higher burden in both GGE and RE syndromes as compared to controls. The detected low-frequency deletions (1) share genes with brain-expressed exons that are under negative selection, (2) overlap with known autism and epilepsy-associated candidate genes, (3) are enriched for CNV intolerant genes recorded by the Exome Aggregation Consortium (ExAC) and (4) coincide with likely disruptive de novo mutations from the NPdenovo database. Employing several knowledge databases, we discuss the most prominent epilepsy candidate genes and their protein-protein networks for GGE and RE.