Probabilistic inference of the genetic architecture underlying functional enrichment of complex traits

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作者
Marion Patxot
Daniel Trejo Banos
Athanasios Kousathanas
Etienne J. Orliac
Sven E. Ojavee
Gerhard Moser
Alexander Holloway
Julia Sidorenko
Zoltan Kutalik
Reedik Mägi
Peter M. Visscher
Lars Rönnegård
Matthew R. Robinson
机构
[1] University of Lausanne,Department of Computational Biology
[2] University of Lausanne,Scientific Computing and Research Support Unit
[3] Australian Agricultural Company Limited,Institute for Molecular Bioscience
[4] University of Queensland,Estonian Genome Center, Institute of Genomics
[5] University Center for Primary Care and Public Health,School of Technology and Business Studies
[6] Swiss Institute of Bioinformatics,Department of Animal Breeding and Genetics
[7] University of Tartu,undefined
[8] Dalarna University,undefined
[9] Swedish University of Agricultural Sciences,undefined
[10] Institute of Science and Technology Austria,undefined
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摘要
We develop a Bayesian model (BayesRR-RC) that provides robust SNP-heritability estimation, an alternative to marker discovery, and accurate genomic prediction, taking 22 seconds per iteration to estimate 8.4 million SNP-effects and 78 SNP-heritability parameters in the UK Biobank. We find that only ≤10% of the genetic variation captured for height, body mass index, cardiovascular disease, and type 2 diabetes is attributable to proximal regulatory regions within 10kb upstream of genes, while 12-25% is attributed to coding regions, 32–44% to introns, and 22-28% to distal 10-500kb upstream regions. Up to 24% of all cis and coding regions of each chromosome are associated with each trait, with over 3,100 independent exonic and intronic regions and over 5,400 independent regulatory regions having ≥95% probability of contributing ≥0.001% to the genetic variance of these four traits. Our open-source software (GMRM) provides a scalable alternative to current approaches for biobank data.
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