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

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 i...

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Autores principales: Fernández-Marmiesse, Ana, Roca, Iria, Díaz-Flores, Felícitas, Cantarín, Verónica, Pérez-Poyato, Mª Socorro, Fontalba, Ana, Laranjeira, Francisco, Quintans, Sofia, Moldovan, Oana, Felgueroso, Blanca, Rodríguez-Pedreira, Montserrat, Simón, Rogelio, Camacho, Ana, Quijada, Pilar, Ibanez-Mico, Salvador, Domingno, Mª Rosario, Benito, Carmen, Calvo, Rocío, Pérez-Cejas, Antonia, Carrasco, Mª Llanos, Ramos, Feliciano, Couce, Mª Luz, Ruiz-Falcó, Mª Luz, Gutierrez-Solana, Luis, Martínez-Atienza, Margarita
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2019
Materias:
Neuroscience
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6856296/
https://www.ncbi.nlm.nih.gov/pubmed/31780880
http://dx.doi.org/10.3389/fnins.2019.01135
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author Fernández-Marmiesse, Ana
Roca, Iria
Díaz-Flores, Felícitas
Cantarín, Verónica
Pérez-Poyato, Mª Socorro
Fontalba, Ana
Laranjeira, Francisco
Quintans, Sofia
Moldovan, Oana
Felgueroso, Blanca
Rodríguez-Pedreira, Montserrat
Simón, Rogelio
Camacho, Ana
Quijada, Pilar
Ibanez-Mico, Salvador
Domingno, Mª Rosario
Benito, Carmen
Calvo, Rocío
Pérez-Cejas, Antonia
Carrasco, Mª Llanos
Ramos, Feliciano
Couce, Mª Luz
Ruiz-Falcó, Mª Luz
Gutierrez-Solana, Luis
Martínez-Atienza, Margarita
author_facet Fernández-Marmiesse, Ana
Roca, Iria
Díaz-Flores, Felícitas
Cantarín, Verónica
Pérez-Poyato, Mª Socorro
Fontalba, Ana
Laranjeira, Francisco
Quintans, Sofia
Moldovan, Oana
Felgueroso, Blanca
Rodríguez-Pedreira, Montserrat
Simón, Rogelio
Camacho, Ana
Quijada, Pilar
Ibanez-Mico, Salvador
Domingno, Mª Rosario
Benito, Carmen
Calvo, Rocío
Pérez-Cejas, Antonia
Carrasco, Mª Llanos
Ramos, Feliciano
Couce, Mª Luz
Ruiz-Falcó, Mª Luz
Gutierrez-Solana, Luis
Martínez-Atienza, Margarita
author_sort Fernández-Marmiesse, Ana
collection PubMed
description 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.
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spelling pubmed-68562962019-11-28 Rare Variants in 48 Genes Account for 42% of Cases of Epilepsy With or Without Neurodevelopmental Delay in 246 Pediatric Patients Fernández-Marmiesse, Ana Roca, Iria Díaz-Flores, Felícitas Cantarín, Verónica Pérez-Poyato, Mª Socorro Fontalba, Ana Laranjeira, Francisco Quintans, Sofia Moldovan, Oana Felgueroso, Blanca Rodríguez-Pedreira, Montserrat Simón, Rogelio Camacho, Ana Quijada, Pilar Ibanez-Mico, Salvador Domingno, Mª Rosario Benito, Carmen Calvo, Rocío Pérez-Cejas, Antonia Carrasco, Mª Llanos Ramos, Feliciano Couce, Mª Luz Ruiz-Falcó, Mª Luz Gutierrez-Solana, Luis Martínez-Atienza, Margarita Front Neurosci Neuroscience 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. Frontiers Media S.A. 2019-11-08 /pmc/articles/PMC6856296/ /pubmed/31780880 http://dx.doi.org/10.3389/fnins.2019.01135 Text en Copyright © 2019 Fernández-Marmiesse, Roca, Díaz-Flores, Cantarín, Pérez-Poyato, Fontalba, Laranjeira, Quintans, Moldovan, Felgueroso, Rodríguez-Pedreira, Simón, Camacho, Quijada, Ibanez-Mico, Domingno, Benito, Calvo, Pérez-Cejas, Carrasco, Ramos, Couce, Ruiz-Falcó, Gutierrez-Solana and Martínez-Atienza. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Neuroscience
Fernández-Marmiesse, Ana
Roca, Iria
Díaz-Flores, Felícitas
Cantarín, Verónica
Pérez-Poyato, Mª Socorro
Fontalba, Ana
Laranjeira, Francisco
Quintans, Sofia
Moldovan, Oana
Felgueroso, Blanca
Rodríguez-Pedreira, Montserrat
Simón, Rogelio
Camacho, Ana
Quijada, Pilar
Ibanez-Mico, Salvador
Domingno, Mª Rosario
Benito, Carmen
Calvo, Rocío
Pérez-Cejas, Antonia
Carrasco, Mª Llanos
Ramos, Feliciano
Couce, Mª Luz
Ruiz-Falcó, Mª Luz
Gutierrez-Solana, Luis
Martínez-Atienza, Margarita
Rare Variants in 48 Genes Account for 42% of Cases of Epilepsy With or Without Neurodevelopmental Delay in 246 Pediatric Patients
title Rare Variants in 48 Genes Account for 42% of Cases of Epilepsy With or Without Neurodevelopmental Delay in 246 Pediatric Patients
title_full Rare Variants in 48 Genes Account for 42% of Cases of Epilepsy With or Without Neurodevelopmental Delay in 246 Pediatric Patients
title_fullStr Rare Variants in 48 Genes Account for 42% of Cases of Epilepsy With or Without Neurodevelopmental Delay in 246 Pediatric Patients
title_full_unstemmed Rare Variants in 48 Genes Account for 42% of Cases of Epilepsy With or Without Neurodevelopmental Delay in 246 Pediatric Patients
title_short Rare Variants in 48 Genes Account for 42% of Cases of Epilepsy With or Without Neurodevelopmental Delay in 246 Pediatric Patients
title_sort rare variants in 48 genes account for 42% of cases of epilepsy with or without neurodevelopmental delay in 246 pediatric patients
topic Neuroscience
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6856296/
https://www.ncbi.nlm.nih.gov/pubmed/31780880
http://dx.doi.org/10.3389/fnins.2019.01135
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