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Multiple causal variants underlie genetic associations in humans

Nathan S. Abell, Marianne K. DeGorter, Michael J. Gloudemans, Emily Greenwald, Kevin S. Smith, Zihuai He, Stephen B. Montgomery

2022Science203 citationsDOIOpen Access PDF

Abstract

Associations between genetic variation and traits are often in noncoding regions with strong linkage disequilibrium (LD), where a single causal variant is assumed to underlie the association. We applied a massively parallel reporter assay (MPRA) to functionally evaluate genetic variants in high, local LD for independent cis-expression quantitative trait loci (eQTL). We found that 17.7% of eQTLs exhibit more than one major allelic effect in tight LD. The detected regulatory variants were highly and specifically enriched for activating chromatin structures and allelic transcription factor binding. Integration of MPRA profiles with eQTL/complex trait colocalizations across 114 human traits and diseases identified causal variant sets demonstrating how genetic association signals can manifest through multiple, tightly linked causal variants.

Topics & Concepts

Expression quantitative trait lociBiologyLinkage disequilibriumGeneticsAlleleQuantitative trait locusGenetic associationGenetic variationGenome-wide association studyChromatinTraitGeneComputational biologyEvolutionary biologyHaplotypeGenotypeSingle-nucleotide polymorphismComputer scienceProgramming languageGenomics and Chromatin DynamicsGenetic Associations and EpidemiologyBioinformatics and Genomic Networks
Multiple causal variants underlie genetic associations in humans | Litcius