Retraction Note: Detection and replication of epistasis influencing transcription in humans

Epistasis has rarely been shown among natural polymorphisms in human traits; this research using advanced computation and gene expression data reveals many instances of epistasis between common single nucleotide polymorphisms in humans, with epistasis and the direction of its effect replicating in independent cohorts. Although frequently demonstrated in model organisms and domesticated species, very few examples of epistasis — where the effect of one polymorphism on a trait depends on other polymorphisms present in the genome — have been demonstrated in humans. Using advanced computation and a gene expression study design, these authors reveal hundreds of instances of epistasis between common single nucleotide polymorphisms (SNPs) in humans. They show that epistasis and direction of its effect replicate in independent cohorts. Epistatic networks of three or more SNPs are shown to influence the expression levels of many genes, whereby one cis-acting SNP is modulated by several trans-acting SNPs. Epistasis is the phenomenon whereby one polymorphism’s effect on a trait depends on other polymorphisms present in the genome. The extent to which epistasis influences complex traits1 and contributes to their variation2,3 is a fundamental question in evolution and human genetics. Although often demonstrated in artificial gene manipulation studies in model organisms4,5, and some examples have been reported in other species6, few examples exist for epistasis among natural polymorphisms in human traits7,8. Its absence from empirical findings may simply be due to low incidence in the genetic control of complex traits2,3, but an alternative view is that it has previously been too technically challenging to detect owing to statistical and computational issues9. Here we show, using advanced computation10 and a gene expression study design, that many instances of epistasis are found between common single nucleotide polymorphisms (SNPs). In a cohort of 846 individuals with 7,339 gene expression levels measured in peripheral blood, we found 501 significant pairwise interactions between common SNPs influencing the expression of 238 genes (P