The phenotypic and genotypic spectrum of epilepsy and intellectual disability in adults: Implications for genetic testing-Reference-Cited by-同舟云学术

The phenotypic and genotypic spectrum of epilepsy and intellectual disability in adults: Implications for genetic testing

Published:2023-03-17 Issue:2 Volume:8 Page:497-508
ISSN:2470-9239
Container-title:Epilepsia Open
language:en
Short-container-title:Epilepsia Open

Author:

von Brauchitsch Sophie¹²,Haslinger Denise²³,Lindlar Silvia²³,Thiele Holger⁴,Bernsen Natalie¹²,Zahnert Felix⁵^ORCID,Reif Philipp S.¹²,Balcik Yunus¹²,Au Ping Yee Billie⁶⁷,Josephson Colin B.⁸⁹¹⁰¹¹¹²^ORCID,Altmüller Janine¹³¹⁴,Strzelczyk Adam¹²^ORCID,Knake Susanne²⁵,Rosenow Felix¹²^ORCID,Chiocchetti Andreas²³,Klein Karl Martin¹²⁶⁷⁸^ORCID

Affiliation:

1. Epilepsy Center Frankfurt Rhine‐Main, Department of Neurology, Center of Neurology and Neurosurgery University Hospital, Goethe‐University Frankfurt Frankfurt am Main Germany

2. Center for Personalized Translational Epilepsy Research (CePTER) Goethe University Frankfurt Frankfurt am Main Germany

3. Department of Child and Adolescent Psychiatry, Psychosomatics and Psychotherapy Goethe University Frankfurt am Main Germany

4. Cologne Center for Genomics (CCG) University of Cologne, Faculty of Medicine and University Hospital Cologne Cologne Germany

5. Epilepsy Center Hessen, Department of Neurology Philipps University Marburg Marburg Germany

6. Department of Medical Genetics, Cumming School of Medicine University of Calgary Alberta Calgary Canada

7. Alberta Children's Hospital Research Institute University of Calgary Alberta Calgary Canada

8. Department of Clinical Neurosciences, Cumming School of Medicine University of Calgary Alberta Calgary Canada

9. Department of Community Health Sciences, Cumming School of Medicine University of Calgary Alberta Calgary Canada

10. Hotchkiss Brain Institute, Cumming School of Medicine University of Calgary Alberta Calgary Canada

11. O’Brien Institute for Public Health University of Calgary Alberta Calgary Canada

12. Centre for Health Informatics University of Calgary Alberta Calgary Canada

13. Berlin Institute of Health at Charité Core Facility Genomics, Universitätsmedizin Berlin Berlin Germany

14. Max Delbrück Center for Molecular Medicine in the Helmholtz Association (MDC) Berlin Germany

Abstract

AbstractObjectiveThe phenotypic and genotypic spectrum of adult patients with epilepsy and intellectual disability (ID) is less clear than in children. We investigated an adult patient cohort to further elucidate this and inform the genetic testing approach.MethodsFifty‐two adult patients (30 male, 22 female) with epilepsy, at least mild ID and no known genetic or acquired cause were included and phenotyped. Variants identified through exome sequencing were evaluated using ACMG criteria. Identified variants were compared with commercially available gene panels. Cluster analysis of two features, age at seizure onset and age at ascertainment of cognitive deficits, was performed.ResultsMedian age was 27 years (range 20‐57 years) with median seizure onset at 3 years and median ascertainment of cognitive deficits at 1 year. Likely pathogenic/pathogenic variants were identified in 16/52 patients (31%) including 14 (27%) single nucleotide variants and 2 (4%) copy number variants. Simulated yield of commercial gene panels varied between 13% in small (≤144 genes) and 27% in large panels (≥1478 genes).Cluster analysis (optimal number 3 clusters) identified a cluster with early seizure onset and early developmental delay (developmental and epileptic encephalopathy, n = 26), a cluster with early developmental delay but late seizure onset (ID with epilepsy, n = 16) and a third cluster with late ascertainment of cognitive deficits and variable seizure onset (n = 7). The smaller gene panels particularly missed the genes identified in the cluster with early ascertainment of cognitive deficits and later onset of epilepsy (0/4) as opposed to the cluster with developmental and epileptic encephalopathy (7/10).SignificanceOur data indicates that adult patients with epilepsy and ID represent a heterogeneous cohort that includes grown‐up patients with DEE but also patients with primary ID and later onset of epilepsy. To maximize diagnostic yield in this cohort either large gene panels or exome sequencing should be used.

Funder

Hessisches Ministerium für Wissenschaft und Kunst

Publisher

Wiley

Subject

Neurology (clinical),Neurology

Link

https://onlinelibrary.wiley.com/doi/pdf/10.1002/epi4.12719

Reference27 articles.

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