Genome-wide Association Study Identifies Genetic Loci for Self-reported Habitual Sleep Duration Supported by Accelerometer-derived Estimates

Overview

Journal Nat Commun

Specialty Biology

Date 2019 Mar 9

PMID 30846698

Citations 269

Authors

Hassan S Dashti

Samuel E Jones

Andrew R Wood

Jacqueline M Lane

Vincent T van Hees

Heming Wang

Jessica A Rhodes

Yanwei Song

Krunal Patel

Simon G Anderson

Robin N Beaumont

David A Bechtold

Jack Bowden

Brian E Cade

Marta Garaulet

Simon D Kyle

Max A Little

Andrew S Loudon

Annemarie I Luik

Frank A J L Scheer

Kai Spiegelhalder

Jessica Tyrrell

Daniel J Gottlieb

Henning Tiemeier

David W Ray

Shaun M Purcell

Timothy M Frayling

Susan Redline

Deborah A Lawlor

Martin K Rutter

Michael N Weedon

Richa Saxena

Affiliations

Soon will be listed here.

Abstract

Sleep is an essential state of decreased activity and alertness but molecular factors regulating sleep duration remain unknown. Through genome-wide association analysis in 446,118 adults of European ancestry from the UK Biobank, we identify 78 loci for self-reported habitual sleep duration (p < 5 × 10; 43 loci at p < 6 × 10). Replication is observed for PAX8, VRK2, and FBXL12/UBL5/PIN1 loci in the CHARGE study (n = 47,180; p < 6.3 × 10), and 55 signals show sign-concordant effects. The 78 loci further associate with accelerometer-derived sleep duration, daytime inactivity, sleep efficiency and number of sleep bouts in secondary analysis (n = 85,499). Loci are enriched for pathways including striatum and subpallium development, mechanosensory response, dopamine binding, synaptic neurotransmission and plasticity, among others. Genetic correlation indicates shared links with anthropometric, cognitive, metabolic, and psychiatric traits and two-sample Mendelian randomization highlights a bidirectional causal link with schizophrenia. This work provides insights into the genetic basis for inter-individual variation in sleep duration implicating multiple biological pathways.

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