학술논문
Efficiently controlling for case-control imbalance and sample relatedness in large-scale genetic association studies
Document Type
Article
Author
Zhou, Wei; Nielsen, Jonas B.; Fritsche, Lars G.; Dey, Rounak; Gabrielsen, Maiken E.; Wolford, Brooke N.; LeFaive, Jonathon; VandeHaar, Peter; Gagliano, Sarah A.; Gifford, Aliya; Bastarache, Lisa A.; Wei, Wei-Qi; Denny, Joshua C.; Lin, Maoxuan; Hveem, Kristian; Kang, Hyun Min; Abecasis, Goncalo R.; Willer, Cristen J.; Lee, Seunggeun
Source
Nature Genetics; September 2018, Vol. 50 Issue: 9 p1335-1341, 7p
Subject
Language
ISSN
10614036; 15461718
Abstract
In genome-wide association studies (GWAS) for thousands of phenotypes in large biobanks, most binary traits have substantially fewer cases than controls. Both of the widely used approaches, the linear mixed model and the recently proposed logistic mixed model, perform poorly; they produce large type I error rates when used to analyze unbalanced case-control phenotypes. Here we propose a scalable and accurate generalized mixed model association test that uses the saddlepoint approximation to calibrate the distribution of score test statistics. This method, SAIGE (Scalable and Accurate Implementation of GEneralized mixed model), provides accurate Pvalues even when case-control ratios are extremely unbalanced. SAIGE uses state-of-art optimization strategies to reduce computational costs; hence, it is applicable to GWAS for thousands of phenotypes by large biobanks. Through the analysis of UK Biobank data of 408,961 samples from white British participants with European ancestry for > 1,400 binary phenotypes, we show that SAIGE can efficiently analyze large sample data, controlling for unbalanced case-control ratios and sample relatedness.