par Hartmann, Corinna;Von Spiczak, Sarah;Muhle, Hiltrud;Stephani, Ulrich;Helbig, Ingo;Suls, Arvid;Weckhuysen, Sarah;de Jonghe, Peter;Buyse, Gunnar;Vilain, Catheline 
;Van Bogaert, Patrick ;Cook, Joseph;Mefford, Heather H.C.
Référence Epilepsia, 56, 3, page (e26-e32)
Publication Publié, 2015-03
;Van Bogaert, Patrick ;Cook, Joseph;Mefford, Heather H.C.Référence Epilepsia, 56, 3, page (e26-e32)
Publication Publié, 2015-03
Article révisé par les pairs
| Résumé : | Fever-associated syndromic epilepsies ranging from febrile seizures plus (FS+) to Dravet syndrome have a significant genetic component. However, apart from SCN1A mutations in >80% of patients with Dravet syndrome, the genetic underpinnings of these epilepsies remain largely unknown. Therefore, we performed a genome-wide screening for copy number variations (CNVs) in 36 patients with SCN1A-negative fever-associated syndromic epilepsies. Phenotypes included Dravet syndrome (n = 23; 64%), genetic epilepsy with febrile seizures plus (GEFS+) and febrile seizures plus (FS+) (n = 11; 31%) and unclassified fever-associated epilepsies (n = 2; 6%). Array comparative genomic hybridization (CGH) was performed using Agilent 4 × 180K arrays. We identified 13 rare CNVs in 8 (22%) of 36 individuals. These included known pathogenic CNVs in 4 (11%) of 36 patients: a 1q21.1 duplication in a proband with Dravet syndrome, a 14q23.3 deletion in a proband with FS+, and two deletions at 16p11.2 and 1q44 in two individuals with fever-associated epilepsy with concomitant autism and/or intellectual disability. In addition, a 3q13.11 duplication in a patient with FS+ and two de novo duplications at 7p14.2 and 18q12.2 in a patient with atypical Dravet syndrome were classified as likely pathogenic. Six CNVs were of unknown significance. The identified genomic aberrations overlap with known neurodevelopmental disorders, suggesting that fever-associated epilepsy syndromes may be a recurrent clinical presentation of known microdeletion syndromes. |
