Dissecting the genetic basis of focal cortical dysplasia: a large cohort study

Genetic malformations of cortical development (MCDs), such as mild MCDs (mMCD), focal cortical dysplasia (FCD), and hemimegalencephaly (HME), are major causes of severe pediatric refractory epilepsies subjected to neurosurgery. FCD2 are characterized by neuropathological hallmarks that include enlar...

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Autores principales: Baldassari, Sara, Ribierre, Théo, Marsan, Elise, Adle-Biassette, Homa, Ferrand-Sorbets, Sarah, Bulteau, Christine, Dorison, Nathalie, Fohlen, Martine, Polivka, Marc, Weckhuysen, Sarah, Dorfmüller, Georg, Chipaux, Mathilde, Baulac, Stéphanie
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Springer Berlin Heidelberg 2019
Materias:
Original Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6851393/
https://www.ncbi.nlm.nih.gov/pubmed/31444548
http://dx.doi.org/10.1007/s00401-019-02061-5
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author Baldassari, Sara
Ribierre, Théo
Marsan, Elise
Adle-Biassette, Homa
Ferrand-Sorbets, Sarah
Bulteau, Christine
Dorison, Nathalie
Fohlen, Martine
Polivka, Marc
Weckhuysen, Sarah
Dorfmüller, Georg
Chipaux, Mathilde
Baulac, Stéphanie
author_facet Baldassari, Sara
Ribierre, Théo
Marsan, Elise
Adle-Biassette, Homa
Ferrand-Sorbets, Sarah
Bulteau, Christine
Dorison, Nathalie
Fohlen, Martine
Polivka, Marc
Weckhuysen, Sarah
Dorfmüller, Georg
Chipaux, Mathilde
Baulac, Stéphanie
author_sort Baldassari, Sara
collection PubMed
description Genetic malformations of cortical development (MCDs), such as mild MCDs (mMCD), focal cortical dysplasia (FCD), and hemimegalencephaly (HME), are major causes of severe pediatric refractory epilepsies subjected to neurosurgery. FCD2 are characterized by neuropathological hallmarks that include enlarged dysmorphic neurons (DNs) and balloon cells (BCs). Here, we provide a comprehensive assessment of the contribution of germline and somatic variants in a large cohort of surgical MCD cases. We enrolled in a monocentric study 80 children with drug-resistant epilepsy and a postsurgical neuropathological diagnosis of mMCD, FCD1, FCD2, or HME. We performed targeted gene sequencing ( ≥ 2000X read depth) on matched blood–brain samples to search for low-allele frequency variants in mTOR pathway and FCD genes. We were able to elucidate 29% of mMCD/FCD1 patients and 63% of FCD2/HME patients. Somatic loss-of-function variants in the N-glycosylation pathway-associated SLC35A2 gene were found in mMCD/FCD1 cases. Somatic gain-of-function variants in MTOR and its activators (AKT3, PIK3CA, RHEB), as well as germline, somatic and two-hit loss-of-function variants in its repressors (DEPDC5, TSC1, TSC2) were found exclusively in FCD2/HME cases. We show that panel-negative FCD2 cases display strong pS6-immunostaining, stressing that all FCD2 are mTORopathies. Analysis of microdissected cells demonstrated that DNs and BCs carry the pathogenic variants. We further observed a correlation between the density of pathological cells and the variant-detection likelihood. Single-cell microdissection followed by sequencing of enriched pools of DNs unveiled a somatic second-hit loss-of-heterozygosity in a DEPDC5 germline case. In conclusion, this study indicates that mMCD/FCD1 and FCD2/HME are two distinct genetic entities: while all FCD2/HME are mosaic mTORopathies, mMCD/FCD1 are not caused by mTOR-pathway-hyperactivating variants, and ~ 30% of the cases are related to glycosylation defects. We provide a framework for efficient genetic testing in FCD/HME, linking neuropathology to genetic findings and emphasizing the usefulness of molecular evaluation in the pediatric epileptic neurosurgical population. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (10.1007/s00401-019-02061-5) contains supplementary material, which is available to authorized users.
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spelling pubmed-68513932019-12-03 Dissecting the genetic basis of focal cortical dysplasia: a large cohort study Baldassari, Sara Ribierre, Théo Marsan, Elise Adle-Biassette, Homa Ferrand-Sorbets, Sarah Bulteau, Christine Dorison, Nathalie Fohlen, Martine Polivka, Marc Weckhuysen, Sarah Dorfmüller, Georg Chipaux, Mathilde Baulac, Stéphanie Acta Neuropathol Original Paper Genetic malformations of cortical development (MCDs), such as mild MCDs (mMCD), focal cortical dysplasia (FCD), and hemimegalencephaly (HME), are major causes of severe pediatric refractory epilepsies subjected to neurosurgery. FCD2 are characterized by neuropathological hallmarks that include enlarged dysmorphic neurons (DNs) and balloon cells (BCs). Here, we provide a comprehensive assessment of the contribution of germline and somatic variants in a large cohort of surgical MCD cases. We enrolled in a monocentric study 80 children with drug-resistant epilepsy and a postsurgical neuropathological diagnosis of mMCD, FCD1, FCD2, or HME. We performed targeted gene sequencing ( ≥ 2000X read depth) on matched blood–brain samples to search for low-allele frequency variants in mTOR pathway and FCD genes. We were able to elucidate 29% of mMCD/FCD1 patients and 63% of FCD2/HME patients. Somatic loss-of-function variants in the N-glycosylation pathway-associated SLC35A2 gene were found in mMCD/FCD1 cases. Somatic gain-of-function variants in MTOR and its activators (AKT3, PIK3CA, RHEB), as well as germline, somatic and two-hit loss-of-function variants in its repressors (DEPDC5, TSC1, TSC2) were found exclusively in FCD2/HME cases. We show that panel-negative FCD2 cases display strong pS6-immunostaining, stressing that all FCD2 are mTORopathies. Analysis of microdissected cells demonstrated that DNs and BCs carry the pathogenic variants. We further observed a correlation between the density of pathological cells and the variant-detection likelihood. Single-cell microdissection followed by sequencing of enriched pools of DNs unveiled a somatic second-hit loss-of-heterozygosity in a DEPDC5 germline case. In conclusion, this study indicates that mMCD/FCD1 and FCD2/HME are two distinct genetic entities: while all FCD2/HME are mosaic mTORopathies, mMCD/FCD1 are not caused by mTOR-pathway-hyperactivating variants, and ~ 30% of the cases are related to glycosylation defects. We provide a framework for efficient genetic testing in FCD/HME, linking neuropathology to genetic findings and emphasizing the usefulness of molecular evaluation in the pediatric epileptic neurosurgical population. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (10.1007/s00401-019-02061-5) contains supplementary material, which is available to authorized users. Springer Berlin Heidelberg 2019-08-23 2019 /pmc/articles/PMC6851393/ /pubmed/31444548 http://dx.doi.org/10.1007/s00401-019-02061-5 Text en © The Author(s) 2019 Open AccessThis article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made.
spellingShingle Original Paper
Baldassari, Sara
Ribierre, Théo
Marsan, Elise
Adle-Biassette, Homa
Ferrand-Sorbets, Sarah
Bulteau, Christine
Dorison, Nathalie
Fohlen, Martine
Polivka, Marc
Weckhuysen, Sarah
Dorfmüller, Georg
Chipaux, Mathilde
Baulac, Stéphanie
Dissecting the genetic basis of focal cortical dysplasia: a large cohort study
title Dissecting the genetic basis of focal cortical dysplasia: a large cohort study
title_full Dissecting the genetic basis of focal cortical dysplasia: a large cohort study
title_fullStr Dissecting the genetic basis of focal cortical dysplasia: a large cohort study
title_full_unstemmed Dissecting the genetic basis of focal cortical dysplasia: a large cohort study
title_short Dissecting the genetic basis of focal cortical dysplasia: a large cohort study
title_sort dissecting the genetic basis of focal cortical dysplasia: a large cohort study
topic Original Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6851393/
https://www.ncbi.nlm.nih.gov/pubmed/31444548
http://dx.doi.org/10.1007/s00401-019-02061-5
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