Systematic visualisation of molecular QTLs reveals variant mechanisms at GWAS loci

Author:

Kerimov NurlanORCID,Tambets Ralf,Hayhurst James D.,Rahu Ida,Kolberg Peep,Raudvere Uku,Kuzmin Ivan,Chowdhary Anshika,Vija Andreas,Teras Hans J.,Kanai MasahiroORCID,Ulirsch Jacob,Ryten Mina,Hardy John,Guelfi Sebastian,Trabzuni Daniah,Kim-Hellmuth Sarah,Rayner Will,Finucane HilaryORCID,Peterson HediORCID,Mosaku AbayomiORCID,Parkinson HelenORCID,Alasoo KaurORCID

Abstract

AbstractSplicing quantitative trait loci (QTLs) have been implicated as a common mechanism underlying complex trait associations. However, utilising splicing QTLs in target discovery and prioritisation has been challenging due to extensive data normalisation which often renders the direction of the genetic effect as well as its magnitude difficult to interpret. This is further complicated by the fact that strong expression QTLs often manifest as weak splicing QTLs and vice versa, making it difficult to uniquely identify the underlying molecular mechanism at each locus. We find that these ambiguities can be mitigated by visualising the association between the genotype and average RNA sequencing read coverage in the region. Here, we generate these QTL coverage plots for 1.7 million molecular QTL associations in the eQTL Catalogue identified with five quantification methods. We illustrate the utility of these QTL coverage plots by performing colocalisation between vitamin D levels in the UK Biobank and all molecular QTLs in the eQTL Catalogue. We find that while visually confirmed splicing QTLs explain just 6/53 of the colocalising signals, they are significantly less pleiotropic than eQTLs and identify a prioritised causal gene in 4/6 cases. All our association summary statistics and QTL coverage plots are freely available athttps://www.ebi.ac.uk/eqtl/.

Publisher

Cold Spring Harbor Laboratory

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