Global discovery of lupus genetic risk variant allelic enhancer activity

Author:

Lu XiaomingORCID,Chen XiaotingORCID,Forney Carmy,Donmez Omer,Miller Daniel,Parameswaran Sreeja,Hong Ted,Huang Yongbo,Pujato Mario,Cazares Tareian,Miraldi Emily R.ORCID,Ray John P.ORCID,de Boer Carl G.ORCID,Harley John B.,Weirauch Matthew T.ORCID,Kottyan Leah C.ORCID

Abstract

AbstractGenome-wide association studies of Systemic Lupus Erythematosus (SLE) nominate 3073 genetic variants at 91 risk loci. To systematically screen these variants for allelic transcriptional enhancer activity, we construct a massively parallel reporter assay (MPRA) library comprising 12,396 DNA oligonucleotides containing the genomic context around every allele of each SLE variant. Transfection into the Epstein-Barr virus-transformed B cell line GM12878 reveals 482 variants with enhancer activity, with 51 variants showing genotype-dependent (allelic) enhancer activity at 27 risk loci. Comparison of MPRA results in GM12878 and Jurkat T cell lines highlights shared and unique allelic transcriptional regulatory mechanisms at SLE risk loci. In-depth analysis of allelic transcription factor (TF) binding at and around allelic variants identifies one class of TFs whose DNA-binding motif tends to be directly altered by the risk variant and a second class of TFs that bind allelically without direct alteration of their motif by the variant. Collectively, our approach provides a blueprint for the discovery of allelic gene regulation at risk loci for any disease and offers insight into the transcriptional regulatory mechanisms underlying SLE.

Publisher

Springer Science and Business Media LLC

Subject

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

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