Common genetic variants contribute to heritability of age at onset of schizophrenia

Author:

Muntané Gerard1ORCID,Sada Ester,Aranda Selena,Martorell Lourdes,Vilella Elisabet1ORCID,Papiol Sergi2ORCID,Heilbronner Urs3ORCID,Schulze Thomas G.4,Kalman Janos5ORCID,Molto Maria Dolores,Aguilar Eduardo,González-Peñas Javier6ORCID,Andreu-Bernabeu Álvaro,Arango Celso7ORCID,Crespo-Facorro Benedicto8,González-Pinto Ana Maria,Fananas Lourdes9ORCID,Arias Bárbara,Bobes Julio10ORCID,Costas Javier11

Affiliation:

1. Hospital Universitari Institut Pere mata

2. University Hospital LMU

3. University Hospital, LMU Munich

4. Ludwig-Maximilians-University Munich

5. Ludwig Maximillians Universitat Muenchen

6. Institute of Psychiatry and Mental Health, Hospital General Universitario Gregorio Marañón, IiSGM, CIBERSAM

7. Institute of Psychiatry and Mental Health, Hospital General Universitario Gregorio Marañón, IiSGM, CIBERSAM, School of Medicine, Universidad Complutense

8. Marqués de Valdecilla University Hospital

9. Universitat de Barcelona

10. Faculty of Medicine and Health Sciences - Universidad de Oviedo

11. Universitario de Santiago

Abstract

AbstractSchizophrenia (SCZ) is a complex disorder that typically arises in late adolescence or early adulthood. Age at onset (AAO) of SCZ is associated with long-term outcomes of the disease. We explored the genetic architecture of AAO with a genome-wide association study (GWAS), heritability, polygenic risk score (PRS), and copy number variant (CNV) analyses in 4 740 subjects of European ancestry. Although no genome-wide significant locus was identified, SNP-based heritability of AAO was estimated to be between 17 and 21%, indicating a moderate contribution of common variants. We also performed cross-trait PRS analyses with a set of mental disorders and identified a negative association between AAO and common variants for Schizophrenia, childhood maltreatment and attention-deficit/hyperactivity disorder. In addition, we explored whether copy number variants (CNVs) previously associated with SCZ played a role in AAO and found that there was no association with earlier onset. To our knowledge, this is the largest GWAS of AAO of SCZ to date, and the first study to determine the involvement of common variants in the heritability of AAO. Finally, we evidenced the role played by higher SCZ load in determining AAO but discarded the role of pathogenic CNVs. Altogether, these results shed light on the genetic architecture of AAO, which needs to be confirmed with larger studies.

Publisher

Research Square Platform LLC

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