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Phenome-wide and expression quantitative trait locus associations of coronavirus disease 2019 genetic risk loci

Chang Moon, Brian M. Schilder, Towfique Raj, Kuan‐lin Huang

2021iScience21 citationsDOIOpen Access PDF

Abstract

While several genes and clinical traits have been associated with higher risk of severe coronavirus disease 2019 (COVID-19), how host genetic variants may interact with these parameters and contribute to severe disease is still unclear. Herein, we performed phenome-wide association study, tissue and immune-cell-specific expression quantitative trait locus (eQTL)/splicing quantitative trait locus, and colocalization analyses for genetic risk loci suggestively associated with severe COVID-19 with respiratory failure. Thirteen phenotypes/traits were associated with the severe COVID-19-associated loci at the genome-wide significance threshold, including monocyte counts, fat metabolism traits, and fibrotic idiopathic interstitial pneumonia. In addition, we identified tissue and immune subtype-specific eQTL associations affecting 48 genes, including several ones that may directly impact host immune responses, colocalized with the severe COVID-19 genome-wide association study associations, and showed altered expression in single-cell transcriptomes. Collectively, our work demonstrates that host genetic variations associated with multiple genes and traits show genetic pleiotropy with severe COVID-19 and may inform disease etiology.

Topics & Concepts

Expression quantitative trait lociBiologyQuantitative trait locusPhenomeGenome-wide association studyGeneticsLocus (genetics)Genetic architectureImmune systemDiseaseGenetic associationGenePhenotypeSingle-nucleotide polymorphismGenotypeMedicinePathologyImmune Cell Function and InteractionSingle-cell and spatial transcriptomicsCOVID-19 Clinical Research Studies