| Literature DB >> 33349701 |
Vivek Chandra1, Sourya Bhattacharyya1, Benjamin J Schmiedel1, Ariel Madrigal1, Cristian Gonzalez-Colin1, Stephanie Fotsing1, Austin Crinklaw1, Gregory Seumois1, Pejman Mohammadi2,3, Mitchell Kronenberg1,4, Bjoern Peters1,5, Ferhat Ay6,7, Pandurangan Vijayanand8,9,10.
Abstract
Expression quantitative trait loci (eQTLs) studies provide associations of genetic variants with gene expression but fall short of pinpointing functionally important eQTLs. Here, using H3K27ac HiChIP assays, we mapped eQTLs overlapping active cis-regulatory elements that interact with their target gene promoters (promoter-interacting eQTLs, pieQTLs) in five common immune cell types (Database of Immune Cell Expression, Expression quantitative trait loci and Epigenomics (DICE) cis-interactome project). This approach allowed us to identify functionally important eQTLs and show mechanisms that explain their cell-type restriction. We also devised an approach to eQTL discovery that relies on HiChIP-based promoter interaction maps as a structural framework for deciding which SNPs to test for association with gene expression, and observe ultra-long-distance pieQTLs (>1 megabase away), including several disease-risk variants. We validated the functional role of pieQTLs using reporter assays, CRISPRi, dCas9-tiling guides and Cas9-mediated base-pair editing. In this article we present a method for functional eQTL discovery and provide insights into relevance of noncoding variants for cell-specific gene regulation and for disease association beyond conventional eQTL mapping.Entities:
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Year: 2020 PMID: 33349701 PMCID: PMC8053422 DOI: 10.1038/s41588-020-00745-3
Source DB: PubMed Journal: Nat Genet ISSN: 1061-4036 Impact factor: 41.307