Integrative modeling of eQTLs and cis-regulatory elements suggest mechanisms underlying cell type specificity of eQTLs

TL;DR

This study integrates eQTL and cis-regulatory element data across multiple cell types to understand the mechanisms behind cell type-specific gene regulation and improve prediction of eQTL effects.

Contribution

It provides a comprehensive analysis of cell type-specific eQTLs and develops a classifier to predict eQTL cell type specificity using CRE data, advancing mechanistic understanding.

Findings

Cis-eQTLs are often cell type specific.

Overlap with CREs predicts eQTL cell type specificity.

A random forest classifier accurately predicts eQTL specificity.

Abstract

Genetic variants in cis-regulatory elements or trans-acting regulators commonly influence the quantity and spatiotemporal distribution of gene transcription. Recent interest in expression quantitative trait locus (eQTL) mapping has paralleled the adoption of genome-wide association studies (GWAS) for the analysis of complex traits and disease in humans. Under the hypothesis that many GWAS associations tag non-coding SNPs with small effects, and that these SNPs exert phenotypic control by modifying gene expression, it has become common to interpret GWAS associations using eQTL data. To exploit the mechanistic interpretability of eQTL-GWAS comparisons, an improved understanding of the genetic architecture and cell type specificity of eQTLs is required. We address this need by performing an eQTL analysis in four parts: first we identified eQTLs from eleven studies on seven cell types; next we quantified cell type specific eQTLs across the studies; then we integrated eQTL data with cis-regulatory element (CRE) data sets from the ENCODE project; finally we built a classifier to predict cell type specific eQTLs. Consistent with prior studies, we demonstrate that allelic heterogeneity is pervasive at cis-eQTLs and that cis-eQTLs are often cell type specific. Within and between cell type eQTL replication is associated with eQTL SNP overlap with hundreds of cell type specific CRE element classes, including enhancer, promoter, and repressive chromatin marks, regions of open chromatin, and many classes of DNA binding proteins. Using a random forest classifier including 526 CRE data sets as features, we successfully predict the cell type specificity of eQTL SNPs in the absence of gene expression data from the cell type of interest. We anticipate that such integrative, predictive modeling will improve our ability to understand the mechanistic basis of human complex phenotypic variation.