Joint Testing of Rare Variant Burden Scores Using Non-negative Least Squares

Overview

Journal Am J Hum Genet

Publisher Cell Press

Specialty Genetics

Date 2024 Oct 4

PMID 39366334

Authors

Andrey Ziyatdinov

Joelle Mbatchou

Anthony Marcketta

Joshua Backman

Sheila Gaynor

Yuxin Zou

Tyler Joseph

Benjamin Geraghty

Joseph Herman

Kyoko Watanabe

Arkopravo Ghosh

Jack Kosmicki

Adam Locke

Timothy Thornton

Hyun Min Kang

Manuel Ferreira

Aris Baras

Goncalo Abecasis

Jonathan Marchini

Affiliations

Soon will be listed here.

Abstract

Gene-based burden tests are a popular and powerful approach for analysis of exome-wide association studies. These approaches combine sets of variants within a gene into a single burden score that is then tested for association. Typically, a range of burden scores are calculated and tested across a range of annotation classes and frequency bins. Correlation between these tests can complicate the multiple testing correction and hamper interpretation of the results. We introduce a method called the sparse burden association test (SBAT) that tests the joint set of burden scores under the assumption that causal burden scores act in the same effect direction. The method simultaneously assesses the significance of the model fit and selects the set of burden scores that best explain the association at the same time. Using simulated data, we show that the method is well calibrated and highlight scenarios where the test outperforms existing gene-based tests. We apply the method to 73 quantitative traits from the UK Biobank, showing that SBAT is a valuable additional gene-based test when combined with other existing approaches. This test is implemented in the REGENIE software.

Citing Articles

Yield of genetic association signals from genomes, exomes and imputation in the UK Biobank.

Gaynor S, Joseph T, Bai X, Zou Y, Boutkov B, Maxwell E Nat Genet. 2024; 56(11):2345-2351.

PMID: 39322778 PMC: 11549045. DOI: 10.1038/s41588-024-01930-4.

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