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Polygenic risk score analysis reveals shared genetic burden between epilepsy and psychiatric comorbidities
Campbell, C.; Lewis-Smith, D.; Leu, C. et al.
2023
 

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2023.07.04.23292071v1.full.pdf
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Mots-clés :
epilepsy
Résumé :
[en] One in three people with epilepsy experiences psychiatric comorbidity, with higher rates in people with drug-resistant epilepsy. Despite their high heritabilities, finding genetic links between epilepsy and psychiatric disorders has proven difficult. We used polygenic risk scoring (PRS) to test whether people with epilepsy have an increased polygenic burden of common genetic variants for depression, anxiety, psychosis, and attention deficit/hyperactivity disorder (ADHD), and examined whether such polygenic burden influences the response to pharmacological treatment of epilepsy.MethodsPhenotype data in the UK Biobank were assessed to identify people with 1) epilepsy (n=8 488), 2) depression (n=143 440), 3) psychosis (n=2 357), 4) ADHD (n=89), and 5) anxiety (n=18 222. Using genotype data and restricting to Caucasian-ancestry samples (n=409 634), PRS for each psychiatric trait were calculated and multinomial regression was used to compare 1) population controls, 2) people with epilepsy and no psychiatric illness, 3) people with epilepsy and the psychiatric trait of interest, and 4) people with the psychiatric trait of interest and no epilepsy. Fixed-effect meta-analysis was used to compare psychiatric PRS in drug-resistant and drug-responsive epilepsy samples from the UK Biobank (n=1 640) and the EpiPGX consortium (n=3 449).ResultsAfter correction for multiple testing, people with epilepsy showed elevated PRS for depression (p<2 x10−16), psychosis (p=0.04) and ADHD (p<0.001). Patients with drug-resistant epilepsy had an increased PRS for psychosis (p=0.002) and depression (p=0.0004) relative to responsive cases.ConclusionWe present evidence that the common genetic basis of epilepsy overlaps with that of psychiatric conditions which are frequently comorbid in people with epilepsy. Common genetic variants that drive psychiatric illness are enriched in people with drug-resistant epilepsy. These results further our understanding of the genetic architecture of epilepsy and suggest a potential future role for polygenic interpretation of common variants in prognostic stratification, both for seizure-treatment outcomes and non-seizure comorbidities.
Centre de recherche :
Luxembourg Centre for Systems Biomedicine (LCSB): Bioinformatics Core (R. Schneider Group)
Disciplines :
Génétique & processus génétiques
Auteur, co-auteur :
Campbell, C.
Lewis-Smith, D.
Leu, C.
Martins, H.
Wolking, S.
KRAUSE, Roland  ;  University of Luxembourg > Luxembourg Centre for Systems Biomedicine (LCSB) > Bioinformatics Core
O’Brien, T.
Sill, G.
Zara, F.
Koeleman, B.
Depondt, C.
Marson, A.
Stefánnson, H.
Stefánnson, K.
Craig, J.
Johnson, MR.
Striano, P.
Jorgensen, A.
Lerche, H.
Delanty, N.
Sisodiya, S.M.
Thomas, R. H.
Cavalleri, G. L. 
Plus d'auteurs (13 en +) Voir moins
Langue du document :
Anglais
Titre :
Polygenic risk score analysis reveals shared genetic burden between epilepsy and psychiatric comorbidities
Date de publication/diffusion :
05 juillet 2023
Source :
Focus Area :
Systems Biomedicine
Objectif de développement durable (ODD) :
3. Bonne santé et bien-être
Projet européen :
FP7 - 279062 - EPIPGX - Epilepsy Pharmacogenomics: delivering biomarkers for clinical use
Intitulé du projet de recherche :
R-AGR-0363 - EpiPGX part UL (01/11/2011 - 21/09/2016) - SCHNEIDER Reinhard
Organisme subsidiant :
Union Européenne
Disponible sur ORBilu :
depuis le 20 octobre 2023

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