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Exploring the phenotypic consequences of tissue specific gene expression variation inferred from GWAS summary statistics

Cited 500 time in Web of Science Cited 511 time in Scopus
Authors

Barbeira, Alvaro N.; Dickinson, Scott P.; Bonazzola, Rodrigo; Zheng, Jiamao; Wheeler, Heather E.; Torres, Jason M.; Torstenson, Eric S.; Shah, Kaanan P.; Garcia, Tzintzuni; Edwards, Todd L.; Stahl, Eli A.; Huckins, Laura M.; Nicolae, Dan L.; Cox, Nancy J.; Im, Hae Kyung; GTEx Consortium; Han, Buhm

Issue Date
2018-12
Publisher
Nature Publishing Group
Citation
Nature Communications, Vol.9, p. 1825
Abstract
© 2018 The Author(s).Scalable, integrative methods to understand mechanisms that link genetic variants with phenotypes are needed. Here we derive a mathematical expression to compute PrediXcan (a gene mapping approach) results using summary data (S-PrediXcan) and show its accuracy and general robustness to misspecified reference sets. We apply this framework to 44 GTEx tissues and 100+ phenotypes from GWAS and meta-analysis studies, creating a growing public catalog of associations that seeks to capture the effects of gene expression variation on human phenotypes. Replication in an independent cohort is shown. Most of the associations are tissue specific, suggesting context specificity of the trait etiology. Colocalized significant associations in unexpected tissues underscore the need for an agnostic scanning of multiple contexts to improve our ability to detect causal regulatory mechanisms. Monogenic disease genes are enriched among significant associations for related traits, suggesting that smaller alterations of these genes may cause a spectrum of milder phenotypes.
ISSN
2041-1723
URI
https://hdl.handle.net/10371/191510
DOI
https://doi.org/10.1038/s41467-018-03621-1
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  • College of Medicine
  • Department of Medicine
Research Area Bioinformatics, Computational Biology, Genomics, Human Leukocyte Antigen, Statistical Genetics

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