Integrative analysis of metabolite GWAS illuminates the molecular basis of pleiotropy and genetic correlation

Author:

Smith Courtney J1ORCID,Sinnott-Armstrong Nasa12ORCID,Cichońska Anna3,Julkunen Heli3ORCID,Fauman Eric B4,Würtz Peter3ORCID,Pritchard Jonathan K15ORCID

Affiliation:

1. Department of Genetics, Stanford University School of Medicine

2. Herbold Computational Biology Program, Fred Hutchinson Cancer Research Center

3. Nightingale Health Plc

4. Internal Medicine Research Unit, Pfizer Worldwide Research, Development and Medical

5. Department of Biology, Stanford University

Abstract

Pleiotropy and genetic correlation are widespread features in genome-wide association studies (GWAS), but they are often difficult to interpret at the molecular level. Here, we perform GWAS of 16 metabolites clustered at the intersection of amino acid catabolism, glycolysis, and ketone body metabolism in a subset of UK Biobank. We utilize the well-documented biochemistry jointly impacting these metabolites to analyze pleiotropic effects in the context of their pathways. Among the 213 lead GWAS hits, we find a strong enrichment for genes encoding pathway-relevant enzymes and transporters. We demonstrate that the effect directions of variants acting on biology between metabolite pairs often contrast with those of upstream or downstream variants as well as the polygenic background. Thus, we find that these outlier variants often reflect biology local to the traits. Finally, we explore the implications for interpreting disease GWAS, underscoring the potential of unifying biochemistry with dense metabolomics data to understand the molecular basis of pleiotropy in complex traits and diseases.

Funder

Stanford Knight-Hennessy Scholars Program

National Science Foundation

National Institute of Health

Publisher

eLife Sciences Publications, Ltd

Subject

General Immunology and Microbiology,General Biochemistry, Genetics and Molecular Biology,General Medicine,General Neuroscience

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