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Mendelian randomization and pathway analysis demonstrate shared genetic associations between lupus and coronary artery disease

Jessica Kain, Katherine A. Owen, Miranda C. Marion, Carl D. Langefeld, Amrie C. Grammer, Peter E. Lipsky

2022Cell Reports Medicine42 citationsDOIOpen Access PDF

Abstract

Coronary artery disease (CAD) is a leading cause of death in patients with systemic lupus erythematosus (SLE). Despite clinical evidence supporting an association between SLE and CAD, pleiotropy-adjusted genetic association studies are limited and focus on only a few common risk loci. Here, we identify a net positive causal estimate of SLE-associated non-HLA SNPs on CAD by traditional Mendelian randomization (MR) approaches. Pathway analysis using SNP-to-gene mapping followed by unsupervised clustering based on protein-protein interactions (PPIs) identifies biological networks composed of positive and negative causal sets of genes. In addition, we confirm the casual effects of specific SNP-to-gene modules on CAD using only SNP mapping to each PPI-defined functional gene set as instrumental variables. This PPI-based MR approach elucidates various molecular pathways with causal implications between SLE and CAD and identifies biological pathways likely causative of both pathologies, revealing known and novel therapeutic interventions for managing CAD in SLE.

Topics & Concepts

Mendelian randomizationCoronary artery diseaseSystemic lupus erythematosusMendelian inheritanceGeneticsDiseaseBiologyMedicineInternal medicineCardiologyComputational biologyGeneGenetic variantsGenotypeSystemic Lupus Erythematosus ResearchAtherosclerosis and Cardiovascular DiseasesLipid metabolism and disorders
Mendelian randomization and pathway analysis demonstrate shared genetic associations between lupus and coronary artery disease | Litcius