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. 2017 Jan;49(1):131-138.
doi: 10.1038/ng.3721. Epub 2016 Dec 5.

Disease variants alter transcription factor levels and methylation of their binding sites

Marc Jan Bonder  1 René Luijk  2 Daria V Zhernakova  1 Matthijs Moed  2 Patrick Deelen  1   3 Martijn Vermaat  4 Maarten van Iterson  2 Freerk van Dijk  1   3 Michiel van Galen  3 Jan Bot  5 Roderick C Slieker  2 P Mila Jhamai  6 Michael Verbiest  3 H Eka D Suchiman  2 Marijn Verkerk  6 Ruud van der Breggen  2 Jeroen van Rooij  6 Nico Lakenberg  2 Wibowo Arindrarto  7 Szymon M Kielbasa  8 Iris Jonkers  1 Peter van 't Hof  8 Irene Nooren  5 Marian Beekman  2 Joris Deelen  2 Diana van Heemst  9 Alexandra Zhernakova  1 Ettje F Tigchelaar  1 Morris A Swertz  1   3 Albert Hofman  10 André G Uitterlinden  6 René Pool  11 Jenny van Dongen  11 Jouke J Hottenga  11 Coen D A Stehouwer  12   13 Carla J H van der Kallen  12   13 Casper G Schalkwijk  12   13 Leonard H van den Berg  14 Erik W van Zwet  7 Hailiang Mei  8 Yang Li  1 Mathieu Lemire  15 Thomas J Hudson  15   16   17 BIOS ConsortiumP Eline Slagboom  2 Cisca Wijmenga  1 Jan H Veldink  14 Marleen M J van Greevenbroek  12   13 Cornelia M van Duijn  18 Dorret I Boomsma  11 Aaron Isaacs  13   18   19 Rick Jansen  20 Joyce B J van Meurs  6 Peter A C 't Hoen  4 Lude Franke  1 Bastiaan T Heijmans  2
Affiliations

Disease variants alter transcription factor levels and methylation of their binding sites

Marc Jan Bonder et al. Nat Genet. 2017 Jan.

Abstract

Most disease-associated genetic variants are noncoding, making it challenging to design experiments to understand their functional consequences. Identification of expression quantitative trait loci (eQTLs) has been a powerful approach to infer the downstream effects of disease-associated variants, but most of these variants remain unexplained. The analysis of DNA methylation, a key component of the epigenome, offers highly complementary data on the regulatory potential of genomic regions. Here we show that disease-associated variants have widespread effects on DNA methylation in trans that likely reflect differential occupancy of trans binding sites by cis-regulated transcription factors. Using multiple omics data sets from 3,841 Dutch individuals, we identified 1,907 established trait-associated SNPs that affect the methylation levels of 10,141 different CpG sites in trans (false discovery rate (FDR) < 0.05). These included SNPs that affect both the expression of a nearby transcription factor (such as NFKB1, CTCF and NKX2-3) and methylation of its respective binding site across the genome. Trans methylation QTLs effectively expose the downstream effects of disease-associated variants.

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