Characterizing substructure via mixture modeling of genetic similarity in large-scale summary statistics

Author:

Stoneman Hayley RORCID,Price Adelle,Trout Nikole Scribner,Lamont Riley,Tifour Souha,Pozdeyev NikitaORCID,Crooks KristyORCID,Lin Meng,Rafaels NicholasORCID,Marker Katie MORCID,Gignoux Christopher RORCID,Henrdicks Audrey EORCID

Abstract

AbstractGenetic summary data are both broadly accessible and highly useful including for risk prediction, causal inference, fine mapping, and the incorporation of external controls. Nevertheless, collapsing individual-level data into groups masks intra- and inter-sample heterogeneity (e.g., population structure), leading to confounding, reduced power, and bias. Unaccounted for substructure limits summary data usability, especially for understudied or admixed populations. Here, we presentSummix2, a comprehensive set of methods and software based on a computationally efficient mixture model of genetic similarity to estimate and adjust for substructure in genetic summary data. In extensive simulations and application to public data,Summix2provides accurate and precise estimates detecting regions of selection, identifying fine-scale population structure, and disentangling latent genetic disease risk.Summix2increases the robust use of diverse publicly available summary data resulting in improved and more equitable research to address population structure, disease etiology, and risk prediction.

Publisher

Cold Spring Harbor Laboratory

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