Discovery and prioritization of variants and genes for kidney function in >1.2 million individuals

Author:

Stanzick Kira J.ORCID,Li YongORCID,Schlosser PascalORCID,Gorski Mathias,Wuttke MatthiasORCID,Thomas Laurent F.ORCID,Rasheed HumairaORCID,Rowan Bryce X.,Graham Sarah E.ORCID,Vanderweff Brett R.,Patil Snehal B.,Robinson-Cohen Cassiane,Gaziano John M.,O’Donnell Christopher J.ORCID,Willer Cristen J.ORCID,Hallan Stein,Åsvold Bjørn OlavORCID,Gessner Andre,Hung Adriana M.,Pattaro CristianORCID,Köttgen AnnaORCID,Stark Klaus J.,Heid Iris M.,Winkler Thomas W.ORCID,

Abstract

AbstractGenes underneath signals from genome-wide association studies (GWAS) for kidney function are promising targets for functional studies, but prioritizing variants and genes is challenging. By GWAS meta-analysis for creatinine-based estimated glomerular filtration rate (eGFR) from the Chronic Kidney Disease Genetics Consortium and UK Biobank (n = 1,201,909), we expand the number of eGFRcrea loci (424 loci, 201 novel; 9.8% eGFRcrea variance explained by 634 independent signal variants). Our increased sample size in fine-mapping (n = 1,004,040, European) more than doubles the number of signals with resolved fine-mapping (99% credible sets down to 1 variant for 44 signals, ≤5 variants for 138 signals). Cystatin-based eGFR and/or blood urea nitrogen association support 348 loci (n = 460,826 and 852,678, respectively). Our customizable tool for Gene PrioritiSation reveals 23 compelling genes including mechanistic insights and enables navigation through genes and variants likely relevant for kidney function in human to help select targets for experimental follow-up.

Funder

Deutsche Forschungsgemeinschaft

Foundation for the National Institutes of Health

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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