Exome sequencing of 20,979 individuals with epilepsy reveals shared and distinct ultra-rare genetic risk across disorder subtypes

Epi25 Collaborative

doi:10.1038/s41593-024-01747-8

Exome sequencing of 20,979 individuals with epilepsy reveals shared and distinct ultra-rare genetic risk across disorder subtypes

Epi25 Collaborative

Broad Institute
University of Melbourne
Massachusetts General Hospital
University of Bonn
University of Luxembourg
Medical University of Vienna
IRCCS Istituto Giannina Gaslini - Genova
University of Genoa
Goethe University Frankfurt
University of Marburg
University College London
Chalfont Centre for Epilepsy
Bezmialem Vakif University
Johns Hopkins University
Dokuz Eylul University
Istanbul University
Nagoya City University
RIKEN
Vanderbilt University
University of Tübingen
University of Aachen
Vivantes Netzwerk für Gesundheit GmbH
Icahn School of Medicine at Mount Sinai
Westchester Medical Center
University of Calgary
Royal College of Surgeons in Ireland
The FutureNeuro Research Centre
Beaumont Hospital, Dublin
Flanders Institute for Biotechnology
University of Antwerp
University of the Witwatersrand
Umeå University
University Hospital of Schleswig-Holstein
DRK-Northern German Epilepsy Centre for Children and Adolescents
Charles University
Azienda Ospedaliero Universitaria Meyer
CHU de Toulouse
The Children's Hospital of Philadelphia
Vilnius University
Marmara University
Chang Gung Memorial Hospital
Monash University
University of Bologna
IRCCS Istituto delle Scienze Neurologiche di Bologna
University of Bristol
University of Eastern Finland
Cyprus Institute of Neurology and Genetics
Magna Græcia University

Research output: Contribution to journal › Article › peer-review

Abstract

Identifying genetic risk factors for highly heterogeneous disorders such as epilepsy remains challenging. Here we present, to our knowledge, the largest whole-exome sequencing study of epilepsy to date, with more than 54,000 human exomes, comprising 20,979 deeply phenotyped patients from multiple genetic ancestry groups with diverse epilepsy subtypes and 33,444 controls, to investigate rare variants that confer disease risk. These analyses implicate seven individual genes, three gene sets and four copy number variants at exome-wide significance. Genes encoding ion channels show strong association with multiple epilepsy subtypes, including epileptic encephalopathies and generalized and focal epilepsies, whereas most other gene discoveries are subtype specific, highlighting distinct genetic contributions to different epilepsies. Combining results from rare single-nucleotide/short insertion and deletion variants, copy number variants and common variants, we offer an expanded view of the genetic architecture of epilepsy, with growing evidence of convergence among different genetic risk loci on the same genes. Top candidate genes are enriched for roles in synaptic transmission and neuronal excitability, particularly postnatally and in the neocortex. We also identify shared rare variant risk between epilepsy and other neurodevelopmental disorders. Our data can be accessed via an interactive browser, hopefully facilitating diagnostic efforts and accelerating the development of follow-up studies.

Original language	English
Pages (from-to)	1864-1879
Number of pages	16
Journal	Nature Neuroscience
Volume	27
Issue number	10
DOIs	https://doi.org/10.1038/s41593-024-01747-8
Publication status	Published - Oct 2024
Externally published	Yes

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SDG 3 Good Health and Well-being

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10.1038/s41593-024-01747-8

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@article{47f81d4954424ffcbbe59b78a733445f,

title = "Exome sequencing of 20,979 individuals with epilepsy reveals shared and distinct ultra-rare genetic risk across disorder subtypes",

abstract = "Identifying genetic risk factors for highly heterogeneous disorders such as epilepsy remains challenging. Here we present, to our knowledge, the largest whole-exome sequencing study of epilepsy to date, with more than 54,000 human exomes, comprising 20,979 deeply phenotyped patients from multiple genetic ancestry groups with diverse epilepsy subtypes and 33,444 controls, to investigate rare variants that confer disease risk. These analyses implicate seven individual genes, three gene sets and four copy number variants at exome-wide significance. Genes encoding ion channels show strong association with multiple epilepsy subtypes, including epileptic encephalopathies and generalized and focal epilepsies, whereas most other gene discoveries are subtype specific, highlighting distinct genetic contributions to different epilepsies. Combining results from rare single-nucleotide/short insertion and deletion variants, copy number variants and common variants, we offer an expanded view of the genetic architecture of epilepsy, with growing evidence of convergence among different genetic risk loci on the same genes. Top candidate genes are enriched for roles in synaptic transmission and neuronal excitability, particularly postnatally and in the neocortex. We also identify shared rare variant risk between epilepsy and other neurodevelopmental disorders. Our data can be accessed via an interactive browser, hopefully facilitating diagnostic efforts and accelerating the development of follow-up studies.",

author = "\{Epi25 Collaborative\} and Berkovic, \{Samuel F.\} and Neale, \{Benjamin M.\} and G{\'a}bor Zsurka and Milena Zizovic and Fritz Zimprich and Federico Zara and Felix Zahnert and Sara Zagaglia and Emrah Y{\"u}cesan and Robert Yolken and Uluc Yis and Zuhal Yapıcı and Kazuhiro Yamakawa and David Wu and \{von Wrede\}, Randi and Isaac Wong and Stefan Wolking and Markus Wolff and Wolf, \{Steven M.\} and Samuel Wiebe and Peter Widdess-Walsh and Sarah Weckhuysen and Weber, \{Yvonne G.\} and Nick Watts and Wagner, \{Ryan G.\} and \{von Spiczak\}, Sarah and \{von Brauchitsch\}, Sophie and Mark{\'e}ta Vl{\v c}kov{\'a} and Annalisa Vetro and Vari, \{Maria Stella\} and \{van Baalen\}, Andreas and Luc Valton and Priya Vaidiswaran and Algirdas Utkus and Sibel Uğur-İ{\c s}eri and Dilsad Turkdogan and Birute Tumiene and Tsai, \{Meng Han\} and Pınar Topaloglu and Marian Todaro and Paolo Tinuper and Timpson, \{Nicholas John\} and Oskari Timonen and Tanteles, \{George A.\} and Taneja, \{Randip S.\} and Talkowski, \{Michael E.\} and Mariagrazia Talarico and Toshimitsu Suzuki and Rainer Surges and Adam Strzelczyk",

note = "Publisher Copyright: {\textcopyright} The Author(s), under exclusive licence to Springer Nature America, Inc. 2024.",

year = "2024",

month = oct,

doi = "10.1038/s41593-024-01747-8",

language = "English",

volume = "27",

pages = "1864--1879",

journal = "Nature Neuroscience",

issn = "1097-6256",

publisher = "Nature Research",

number = "10",

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T1 - Exome sequencing of 20,979 individuals with epilepsy reveals shared and distinct ultra-rare genetic risk across disorder subtypes

AU - Epi25 Collaborative

AU - Berkovic, Samuel F.

AU - Neale, Benjamin M.

AU - Zsurka, Gábor

AU - Zizovic, Milena

AU - Zimprich, Fritz

AU - Zara, Federico

AU - Zahnert, Felix

AU - Zagaglia, Sara

AU - Yücesan, Emrah

AU - Yolken, Robert

AU - Yis, Uluc

AU - Yapıcı, Zuhal

AU - Yamakawa, Kazuhiro

AU - Wu, David

AU - von Wrede, Randi

AU - Wong, Isaac

AU - Wolking, Stefan

AU - Wolff, Markus

AU - Wolf, Steven M.

AU - Wiebe, Samuel

AU - Widdess-Walsh, Peter

AU - Weckhuysen, Sarah

AU - Weber, Yvonne G.

AU - Watts, Nick

AU - Wagner, Ryan G.

AU - von Spiczak, Sarah

AU - von Brauchitsch, Sophie

AU - Vlčková, Markéta

AU - Vetro, Annalisa

AU - Vari, Maria Stella

AU - van Baalen, Andreas

AU - Valton, Luc

AU - Vaidiswaran, Priya

AU - Utkus, Algirdas

AU - Uğur-İşeri, Sibel

AU - Turkdogan, Dilsad

AU - Tumiene, Birute

AU - Tsai, Meng Han

AU - Topaloglu, Pınar

AU - Todaro, Marian

AU - Tinuper, Paolo

AU - Timpson, Nicholas John

AU - Timonen, Oskari

AU - Tanteles, George A.

AU - Taneja, Randip S.

AU - Talkowski, Michael E.

AU - Talarico, Mariagrazia

AU - Suzuki, Toshimitsu

AU - Surges, Rainer

AU - Strzelczyk, Adam

PY - 2024/10

Y1 - 2024/10

N2 - Identifying genetic risk factors for highly heterogeneous disorders such as epilepsy remains challenging. Here we present, to our knowledge, the largest whole-exome sequencing study of epilepsy to date, with more than 54,000 human exomes, comprising 20,979 deeply phenotyped patients from multiple genetic ancestry groups with diverse epilepsy subtypes and 33,444 controls, to investigate rare variants that confer disease risk. These analyses implicate seven individual genes, three gene sets and four copy number variants at exome-wide significance. Genes encoding ion channels show strong association with multiple epilepsy subtypes, including epileptic encephalopathies and generalized and focal epilepsies, whereas most other gene discoveries are subtype specific, highlighting distinct genetic contributions to different epilepsies. Combining results from rare single-nucleotide/short insertion and deletion variants, copy number variants and common variants, we offer an expanded view of the genetic architecture of epilepsy, with growing evidence of convergence among different genetic risk loci on the same genes. Top candidate genes are enriched for roles in synaptic transmission and neuronal excitability, particularly postnatally and in the neocortex. We also identify shared rare variant risk between epilepsy and other neurodevelopmental disorders. Our data can be accessed via an interactive browser, hopefully facilitating diagnostic efforts and accelerating the development of follow-up studies.

AB - Identifying genetic risk factors for highly heterogeneous disorders such as epilepsy remains challenging. Here we present, to our knowledge, the largest whole-exome sequencing study of epilepsy to date, with more than 54,000 human exomes, comprising 20,979 deeply phenotyped patients from multiple genetic ancestry groups with diverse epilepsy subtypes and 33,444 controls, to investigate rare variants that confer disease risk. These analyses implicate seven individual genes, three gene sets and four copy number variants at exome-wide significance. Genes encoding ion channels show strong association with multiple epilepsy subtypes, including epileptic encephalopathies and generalized and focal epilepsies, whereas most other gene discoveries are subtype specific, highlighting distinct genetic contributions to different epilepsies. Combining results from rare single-nucleotide/short insertion and deletion variants, copy number variants and common variants, we offer an expanded view of the genetic architecture of epilepsy, with growing evidence of convergence among different genetic risk loci on the same genes. Top candidate genes are enriched for roles in synaptic transmission and neuronal excitability, particularly postnatally and in the neocortex. We also identify shared rare variant risk between epilepsy and other neurodevelopmental disorders. Our data can be accessed via an interactive browser, hopefully facilitating diagnostic efforts and accelerating the development of follow-up studies.

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DO - 10.1038/s41593-024-01747-8

M3 - Article

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AN - SCOPUS:85205532641

SN - 1097-6256

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EP - 1879

JO - Nature Neuroscience

JF - Nature Neuroscience

IS - 10

ER -

Exome sequencing of 20,979 individuals with epilepsy reveals shared and distinct ultra-rare genetic risk across disorder subtypes

Abstract

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