Identification of novel genomic risk loci shared between common epilepsies and psychiatric disorders

Psychiatric disorders and common epilepsies are heritable disorders with a high comorbidity and overlapping symptoms. However, the causative mechanisms underlying this relationship are poorly understood. Here we aimed to identify overlapping genetic loci between epilepsy and psychiatric disorders to...

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Autores principales: Karadag, Naz, Shadrin, Alexey A, O’Connell, Kevin S, Hindley, Guy F L, Rahman, Zillur, Parker, Nadine, Bahrami, Shahram, Fominykh, Vera, Cheng, Weiqiu, Holen, Børge, Alvestad, Silje, Taubøll, Erik, Steen, Nils Eiel, Djurovic, Srdjan, Dale, Anders M, Frei, Oleksandr, Andreassen, Ole A, Smeland, Olav B
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2023
Materias:
Original Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10393410/
https://www.ncbi.nlm.nih.gov/pubmed/36757824
http://dx.doi.org/10.1093/brain/awad038
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author Karadag, Naz
Shadrin, Alexey A
O’Connell, Kevin S
Hindley, Guy F L
Rahman, Zillur
Parker, Nadine
Bahrami, Shahram
Fominykh, Vera
Cheng, Weiqiu
Holen, Børge
Alvestad, Silje
Taubøll, Erik
Steen, Nils Eiel
Djurovic, Srdjan
Dale, Anders M
Frei, Oleksandr
Andreassen, Ole A
Smeland, Olav B
author_facet Karadag, Naz
Shadrin, Alexey A
O’Connell, Kevin S
Hindley, Guy F L
Rahman, Zillur
Parker, Nadine
Bahrami, Shahram
Fominykh, Vera
Cheng, Weiqiu
Holen, Børge
Alvestad, Silje
Taubøll, Erik
Steen, Nils Eiel
Djurovic, Srdjan
Dale, Anders M
Frei, Oleksandr
Andreassen, Ole A
Smeland, Olav B
author_sort Karadag, Naz
collection PubMed
description Psychiatric disorders and common epilepsies are heritable disorders with a high comorbidity and overlapping symptoms. However, the causative mechanisms underlying this relationship are poorly understood. Here we aimed to identify overlapping genetic loci between epilepsy and psychiatric disorders to gain a better understanding of their comorbidity and shared clinical features. We analysed genome-wide association study data for all epilepsies (n = 44 889), genetic generalized epilepsy (n = 33 446), focal epilepsy (n = 39 348), schizophrenia (n = 77 096), bipolar disorder (n = 406 405), depression (n = 500 199), attention deficit hyperactivity disorder (n = 53 293) and autism spectrum disorder (n = 46 350). First, we applied the MiXeR tool to estimate the total number of causal variants influencing the disorders. Next, we used the conjunctional false discovery rate statistical framework to improve power to discover shared genomic loci. Additionally, we assessed the validity of the findings in independent cohorts, and functionally characterized the identified loci. The epilepsy phenotypes were considerably less polygenic (1.0 K to 3.4 K causal variants) than the psychiatric disorders (5.6 K to 13.9 K causal variants), with focal epilepsy being the least polygenic (1.0 K variants), and depression having the highest polygenicity (13.9 K variants). We observed cross-trait genetic enrichment between genetic generalized epilepsy and all psychiatric disorders and between all epilepsies and schizophrenia and depression. Using conjunctional false discovery rate analysis, we identified 40 distinct loci jointly associated with epilepsies and psychiatric disorders at conjunctional false discovery rate <0.05, four of which were associated with all epilepsies and 39 with genetic generalized epilepsy. Most epilepsy risk loci were shared with schizophrenia (n = 31). Among the identified loci, 32 were novel for genetic generalized epilepsy, and two were novel for all epilepsies. There was a mixture of concordant and discordant allelic effects in the shared loci. The sign concordance of the identified variants was highly consistent between the discovery and independent datasets for all disorders, supporting the validity of the findings. Gene-set analysis for the shared loci between schizophrenia and genetic generalized epilepsy implicated biological processes related to cell cycle regulation, protein phosphatase activity, and membrane and vesicle function; the gene-set analyses for the other loci were underpowered. The extensive genetic overlap with mixed effect directions between psychiatric disorders and common epilepsies demonstrates a complex genetic relationship between these disorders, in line with their bi-directional relationship, and indicates that overlapping genetic risk may contribute to shared pathophysiological and clinical features between epilepsy and psychiatric disorders.
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spelling pubmed-103934102023-08-02 Identification of novel genomic risk loci shared between common epilepsies and psychiatric disorders Karadag, Naz Shadrin, Alexey A O’Connell, Kevin S Hindley, Guy F L Rahman, Zillur Parker, Nadine Bahrami, Shahram Fominykh, Vera Cheng, Weiqiu Holen, Børge Alvestad, Silje Taubøll, Erik Steen, Nils Eiel Djurovic, Srdjan Dale, Anders M Frei, Oleksandr Andreassen, Ole A Smeland, Olav B Brain Original Article Psychiatric disorders and common epilepsies are heritable disorders with a high comorbidity and overlapping symptoms. However, the causative mechanisms underlying this relationship are poorly understood. Here we aimed to identify overlapping genetic loci between epilepsy and psychiatric disorders to gain a better understanding of their comorbidity and shared clinical features. We analysed genome-wide association study data for all epilepsies (n = 44 889), genetic generalized epilepsy (n = 33 446), focal epilepsy (n = 39 348), schizophrenia (n = 77 096), bipolar disorder (n = 406 405), depression (n = 500 199), attention deficit hyperactivity disorder (n = 53 293) and autism spectrum disorder (n = 46 350). First, we applied the MiXeR tool to estimate the total number of causal variants influencing the disorders. Next, we used the conjunctional false discovery rate statistical framework to improve power to discover shared genomic loci. Additionally, we assessed the validity of the findings in independent cohorts, and functionally characterized the identified loci. The epilepsy phenotypes were considerably less polygenic (1.0 K to 3.4 K causal variants) than the psychiatric disorders (5.6 K to 13.9 K causal variants), with focal epilepsy being the least polygenic (1.0 K variants), and depression having the highest polygenicity (13.9 K variants). We observed cross-trait genetic enrichment between genetic generalized epilepsy and all psychiatric disorders and between all epilepsies and schizophrenia and depression. Using conjunctional false discovery rate analysis, we identified 40 distinct loci jointly associated with epilepsies and psychiatric disorders at conjunctional false discovery rate <0.05, four of which were associated with all epilepsies and 39 with genetic generalized epilepsy. Most epilepsy risk loci were shared with schizophrenia (n = 31). Among the identified loci, 32 were novel for genetic generalized epilepsy, and two were novel for all epilepsies. There was a mixture of concordant and discordant allelic effects in the shared loci. The sign concordance of the identified variants was highly consistent between the discovery and independent datasets for all disorders, supporting the validity of the findings. Gene-set analysis for the shared loci between schizophrenia and genetic generalized epilepsy implicated biological processes related to cell cycle regulation, protein phosphatase activity, and membrane and vesicle function; the gene-set analyses for the other loci were underpowered. The extensive genetic overlap with mixed effect directions between psychiatric disorders and common epilepsies demonstrates a complex genetic relationship between these disorders, in line with their bi-directional relationship, and indicates that overlapping genetic risk may contribute to shared pathophysiological and clinical features between epilepsy and psychiatric disorders. Oxford University Press 2023-02-09 /pmc/articles/PMC10393410/ /pubmed/36757824 http://dx.doi.org/10.1093/brain/awad038 Text en © The Author(s) 2023. Published by Oxford University Press on behalf of the Guarantors of Brain. https://creativecommons.org/licenses/by-nc/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution-NonCommercial License (https://creativecommons.org/licenses/by-nc/4.0/), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is properly cited. For commercial re-use, please contact journals.permissions@oup.com
spellingShingle Original Article
Karadag, Naz
Shadrin, Alexey A
O’Connell, Kevin S
Hindley, Guy F L
Rahman, Zillur
Parker, Nadine
Bahrami, Shahram
Fominykh, Vera
Cheng, Weiqiu
Holen, Børge
Alvestad, Silje
Taubøll, Erik
Steen, Nils Eiel
Djurovic, Srdjan
Dale, Anders M
Frei, Oleksandr
Andreassen, Ole A
Smeland, Olav B
Identification of novel genomic risk loci shared between common epilepsies and psychiatric disorders
title Identification of novel genomic risk loci shared between common epilepsies and psychiatric disorders
title_full Identification of novel genomic risk loci shared between common epilepsies and psychiatric disorders
title_fullStr Identification of novel genomic risk loci shared between common epilepsies and psychiatric disorders
title_full_unstemmed Identification of novel genomic risk loci shared between common epilepsies and psychiatric disorders
title_short Identification of novel genomic risk loci shared between common epilepsies and psychiatric disorders
title_sort identification of novel genomic risk loci shared between common epilepsies and psychiatric disorders
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10393410/
https://www.ncbi.nlm.nih.gov/pubmed/36757824
http://dx.doi.org/10.1093/brain/awad038
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