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Rare Variants in 48 Genes Account for 42% of Cases of Epilepsy With or Without Neurodevelopmental Delay in 246 Pediatric Patients

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dc.contributor.author Fernández-Marmiesse, Ana
dc.contributor.author Roca, Iria
dc.contributor.author Díaz-Flores, Felicitas
dc.contributor.author Cantarin, Veronica
dc.contributor.author Socorro-Pérez-Poyato, Ma
dc.contributor.author Fontalba, Ana
dc.contributor.author Laranjeira, Francisco
dc.contributor.author Quintans, Sofia
dc.contributor.author Moldovan, Oana
dc.contributor.author Felgueroso, Blanca
dc.contributor.author Rodríguez-Pedreira, Montserrat
dc.contributor.author Simon, Rogelio
dc.contributor.author Camacho, Ana
dc.contributor.author Quijada, Pilar
dc.contributor.author Ibáñez-Mico, Salvador
dc.contributor.author Rosario-Domingno, Ma
dc.contributor.author Benito, Carmen
dc.contributor.author Calvo, Rocío
dc.contributor.author Pérez-Cejas, Antonia
dc.contributor.author Llanos-Carrasco, Ma
dc.contributor.author Ramos, Feliciano
dc.contributor.author Luz-Couce, Ma
dc.contributor.author Luz-Ruiz-Falco, Ma
dc.contributor.author Gutiérrez-Solana, Luis
dc.contributor.author Martínez-Atienza, Margarita
dc.date.accessioned 2026-01-19T16:08:06Z
dc.date.available 2026-01-19T16:08:06Z
dc.date.issued 2019-11-08
dc.identifier.citation Fernández-Marmiesse A, Roca I, Díaz-Flores F, Cantarín V, Pérez-Poyato MS, Fontalba A, et al. Rare Variants in 48 Genes Account for 42% of Cases of Epilepsy With or Without Neurodevelopmental Delay in 246 Pediatric Patients. Front Neurosci. 8 de noviembre de 2019;13:1135.
dc.identifier.uri https://sms.carm.es/ricsmur/handle/123456789/23752
dc.description.abstract In order to characterize the genetic architecture of epilepsy in a pediatric population from the Iberian Peninsula (including the Canary Islands), we conducted targeted exome sequencing of 246 patients with infantile-onset seizures with or without neurodevelopmental delay. We detected 107 variants in 48 different genes, which were implicated in neuronal excitability, neurodevelopment, synaptic transmission, and metabolic pathways. In 104 cases (42%) we detected variant(s) that we classified as pathogenic or likely pathogenic. Of the 48 mutated genes, 32 were dominant, 8 recessive and 8 X-linked. Of the patients for whom family studies could be performed and in whom pathogenic variants were identified in dominant or X-linked genes, 82% carried de novo mutations. The involvement of small copy number variations (CNVs) is 9%. The use of progressively updated custom panels with high mean vertical coverage enabled establishment of a definitive diagnosis in a large proportion of cases (42%) and detection of CNVs (even duplications) with high fidelity. In 10.5% of patients we detected associations that are pending confirmation via functional and/or familial studies. Our findings had important consequences for the clinical management of the probands, since a large proportion of the cohort had been clinically misdiagnosed, and their families were subsequently able to avail of genetic counseling. In some cases, a more appropriate treatment was selected for the patient in question, or an inappropriate treatment discontinued. Our findings suggest the existence of modifier genes that may explain the incomplete penetrance of some epilepsy-related genes. We discuss possible reasons for non-diagnosis and future research directions. Further studies will be required to uncover the roles of structural variants, epimutations, and oligogenic inheritance in epilepsy, thereby providing a more complete molecular picture of this disease. In summary, given the broad phenotypic spectrum of most epilepsy-related genes, efficient genomic tools like the targeted exome sequencing panel described here are essential for early diagnosis and treatment, and should be implemented as first-tier diagnostic tools for children with epilepsy without a clear etiologic basis.
dc.language.iso eng
dc.publisher FRONTIERS MEDIA SA
dc.rights Atribución/Reconocimiento 4.0 Internacional
dc.rights.uri https://creativecommons.org/licenses/by/4.0/deed.es *
dc.title Rare Variants in 48 Genes Account for 42% of Cases of Epilepsy With or Without Neurodevelopmental Delay in 246 Pediatric Patients
dc.type info:eu-repo/semantics/article
dc.identifier.pmid 31780880
dc.relation.publisherversion https://www.frontiersin.org/article/10.3389/fnins.2019.01135/full
dc.type.version info:eu-repo/semantics/publishedVersion
dc.identifier.doi 10.3389/fnins.2019.01135
dc.journal.title Frontiers in Neuroscience
dc.identifier.essn 1662-453X


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