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A Genome-wide Association Study of Early Menopause and the Combined Impact of Identified Variants

Overview
Journal Hum Mol Genet
Specialties Genetics
Molecular Biology
Date 2013 Jan 12
PMID 23307926
Citations 49
Authors
John R B Perry
Tanguy Corre
Tonu Esko
Daniel I Chasman
Krista Fischer
Nora Franceschini
Chunyan He
Zoltan Kutalik
Massimo Mangino
Lynda M Rose
Albert Vernon Smith
Lisette Stolk
Patrick Sulem
Michael N Weedon
Wei V Zhuang
Alice Arnold
Alan Ashworth
Sven Bergmann
Julie E Buring
Andrea Burri
Constance Chen
Marilyn C Cornelis
David J Couper
Mark O Goodarzi
Vilmundur Gudnason
Tamara Harris
Albert Hofman
Michael Jones
Peter Kraft
Lenore Launer
Joop S E Laven
Guo Li
Barbara McKnight
Corrado Masciullo
Lili Milani
Nicholas Orr
Bruce M Psaty
Paul M Ridker
Fernando Rivadeneira
Cinzia Sala
Andres Salumets
Minouk Schoemaker
Michela Traglia
Gerard Waeber
Stephen J Chanock
Ellen W Demerath
Melissa Garcia
Susan E Hankinson
Frank B Hu
David J Hunter
Kathryn L Lunetta
Andres Metspalu
Grant W Montgomery
Joanne M Murabito
Anne B Newman
Ken K Ong
Tim D Spector
Kari Stefansson
Anthony J Swerdlow
Unnur Thorsteinsdottir
Rob M van Dam
Andre G Uitterlinden
Jenny A Visser
Peter Vollenweider
Daniela Toniolo
Anna Murray
Affiliations
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Abstract

Early menopause (EM) affects up to 10% of the female population, reducing reproductive lifespan considerably. Currently, it constitutes the leading cause of infertility in the western world, affecting mainly those women who postpone their first pregnancy beyond the age of 30 years. The genetic aetiology of EM is largely unknown in the majority of cases. We have undertaken a meta-analysis of genome-wide association studies (GWASs) in 3493 EM cases and 13 598 controls from 10 independent studies. No novel genetic variants were discovered, but the 17 variants previously associated with normal age at natural menopause as a quantitative trait (QT) were also associated with EM and primary ovarian insufficiency (POI). Thus, EM has a genetic aetiology which overlaps variation in normal age at menopause and is at least partly explained by the additive effects of the same polygenic variants. The combined effect of the common variants captured by the single nucleotide polymorphism arrays was estimated to account for ∼30% of the variance in EM. The association between the combined 17 variants and the risk of EM was greater than the best validated non-genetic risk factor, smoking.

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