Leveraging both individual-level genetic data and GWAS summary statistics increases polygenic prediction
By
Clara Albiñana,
Jakob Grove,
John J. McGrath,
Esben Agerbo,
Naomi R. Wray,
Thomas Werge,
Anders D Børglum,
Preben Bo Mortensen,
Florian Privé,
Bjarni J Vilhjálmsson
Posted 27 Nov 2020
bioRxiv DOI: 10.1101/2020.11.27.401141
The accuracy of polygenic risk scores (PRSs) to predict complex diseases increases with the training sample size. PRSs are generally derived based on summary statistics from large meta-analyses of multiple genome-wide association studies (GWAS). However, it is now common for researchers to have access to large individual-level data as well, such as the UK biobank data. To the best of our knowledge, it has not yet been explored how to best combine both types of data (summary statistics and individual-level data) to optimize polygenic prediction. The most widely used approach to combine data is the meta-analysis of GWAS summary statistics (Meta-GWAS), but we show that it does not always provide the most accurate PRS. Through simulations and using twelve real case-control and quantitative traits from both iPSYCH and UK Biobank along with external GWAS summary statistics, we compare Meta-GWAS with two alternative data-combining approaches, stacked clumping and thresholding (SCT) and Meta-PRS. We find that, when large individual-level data is available, the linear combination of PRSs (Meta-PRS) is both a simple alternative to Meta-GWAS and often more accurate.
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