Many genetic variants associated with common disease susceptibility occur close to immune-related genes in noncoding DNA, suggestive of a regulatory function. The definition of functional variants and the specific genes that they regulate remains challenging and in many cases is unresolved. We hypothesized that a significant proportion of variants, including those implicated in disease, may show activity in a context-specific manner and therefore only be identifiable upon triggering of immune responses.

Context-specific genetic association with differential gene expression in IFN-β signaling. (A) A local association (cis-eQTL) with IFNB1 expression for a single-nucleotide polymorphism (rs2275888) revealed after 2 hours of LPS stimulation of monocytes. (B) This genetic marker shows association with expression of 17 genes on different chromosomes (trans-eQTLs) after 24 hours of LPS stimulation, forming a gene network (C) consistent with the IFN-β signaling cascade.

We mapped interindividual variation in gene expression as a quantitative trait, defining expression quantitative trait loci (eQTLs). To investigate the effect of innate immune stimuli on eQTLs, we exposed primary CD14⁺ human monocytes from 432 European volunteers to the inflammatory proxies interferon-γ (IFN-γ) or differing durations (2 or 24 hours) of lipopolysaccharide (LPS). eQTL mapping was performed on a genome-wide basis with an additive linear model. A subset of 228 individuals with expression data available for all experimental conditions enabled cross-treatment comparisons.

Stimulation with LPS or IFN-γ resulted in profound effects across monocyte eQTLs, with hundreds of genes and associated pathways demonstrating context-specific eQTLs dependent on the type and duration of stimulus. Context-specific eQTLs frequently intersected established canonical pathways of monocyte signaling and included key nodal genes and effector molecules. These eQTLs are typically more distal to the transcriptional start site and, in some cases, showed reversal of effect between conditions. We also found stimulation reveals novel eQTLs with simultaneous effects involving many genes (trans-eQTLs). Examples included coding polymorphisms in CYP1B1, P2RY11, and IDO2 that modulate activity and develop trans network effects upon stimulation; an LPS-specific IFN-β cytokine network response driven by a cis-eQTL for IFNB1 that was only revealed over time; an interferon regulatory factor 2 (IRF2) transcription factor modulated network up-regulated by IFN-γ involving a cis-eQTL for IRF2; and an IFN-γ–inducible trans gene network involving the transcription factor NFE2L3. We find trans associations to the major histocompatibility complex are dependent on context, paralleling the expression of class II genes. Induced eQTLs were enriched for disease-risk loci with context-specific associations to many putative causal genes, including at ATM, IRF8, and CCR3. Conditional analysis defined additional independent stimulus-specific peaks of association for a given gene. For CARD9 we observed, in addition to a constitutive eQTL informative for a genome-wide association study locus for Crohn’s disease, a stimulus-specific peak eQTL after IFN-γ, defining a further independent signal of disease association.

Interindividual variation in immune responses is accompanied by diverging patterns of gene regulation dependent on underlying genotype. In human monocytes, many regulatory variants display functionality only after pathophysiologically relevant immune stimuli. By considering the cellular and environmental context relevant to disease, it is …