Identification of atrial fibrillation associated genes and functional non-coding variants

Antoinette F. van Ouwerkerk(Amsterdam UMC Location University of Amsterdam), Fernanda M. Bosada(Amsterdam UMC Location University of Amsterdam), Karel van Duijvenboden(Amsterdam UMC Location University of Amsterdam), Matthew C. Hill(Baylor College of Medicine), Lindsey E. Montefiori(University of Chicago), Koen T. Scholman(Amsterdam UMC Location University of Amsterdam), Jia Liu(Leiden University Medical Center), Antoine A.F. de Vries(Leiden University Medical Center), Bastiaan J. Boukens(Amsterdam UMC Location University of Amsterdam), Patrick T. Ellinor(Broad Institute), Marie‐José Goumans(Leiden University Medical Center), Igor R. Efimov(George Washington University), Marcelo A. Nóbrega(University of Chicago), Phil Barnett(Amsterdam UMC Location University of Amsterdam), James F. Martin(Baylor College of Medicine), Vincent M. Christoffels(Amsterdam UMC Location University of Amsterdam)
Nature Communications
October 18, 2019
Cited by 92Open Access
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Abstract

Disease-associated genetic variants that lie in non-coding regions found by genome-wide association studies are thought to alter the functionality of transcription regulatory elements and target gene expression. To uncover causal genetic variants, variant regulatory elements and their target genes, here we cross-reference human transcriptomic, epigenomic and chromatin conformation datasets. Of 104 genetic variant regions associated with atrial fibrillation candidate target genes are prioritized. We optimize EMERGE enhancer prediction and use accessible chromatin profiles of human atrial cardiomyocytes to more accurately predict cardiac regulatory elements and identify hundreds of sub-threshold variants that co-localize with regulatory elements. Removal of mouse homologues of atrial fibrillation-associated regions in vivo uncovers a distal regulatory region involved in Gja1 (Cx43) expression. Our analyses provide a shortlist of genes likely affected by atrial fibrillation-associated variants and provide variant regulatory elements in each region that link genetic variation and target gene regulation, helping to focus future investigations.


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