Affiliation:
1. Centre for Neuroimaging, Cognition and Genomics, School of Biological and Chemical Sciences University of Galway Galway Ireland
2. Department of Biology Maynooth University Maynooth Ireland
Abstract
AbstractGenome‐wide association studies (GWAS) have been important for characterizing the genetic component and enhancing our understanding of the biological aetiology of both neuropsychiatric disorders and sleep‐related phenotypes such as chronotype, which is our preference for morning or evening time. Mendelian randomization (MR) is a post‐GWAS analysis that is used to infer causal relationships between potential risk factors and outcomes. MR uses genetic variants as instrumental variants for exposures to study the effect on outcomes. This review details the main results from GWAS of neuropsychiatric disorders and sleep‐related phenotypes, and the application of MR to investigate their bidirectional relationship. The main results from MR studies of neuropsychiatric disorders and sleep‐related phenotypes are summarized. These MR studies have identified 37 causal relationships between neuropsychiatric disorders and sleep‐related phenotypes. MR studies identified evidence of a causal role for five neuropsychiatric disorders and symptoms (attention deficit hyperactivity disorder, bipolar disorder, depressive symptoms, major depressive disorder and schizophrenia) on sleep‐related phenotypes and evidence of a causal role for five sleep‐related phenotypes (daytime napping, insomnia, morning person, long sleep duration and sleep duration) on risk for neuropsychiatric disorders. These MR results show a bidirectional relationship between neuropsychiatric disorders and sleep‐related phenotypes and identify potential risk factors for follow‐up studies.
Funder
European Research Council
Science Foundation Ireland
Cited by
1 articles.
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