Genetic influences on circulating retinol and its relationship to human health

Author:

Reay William R.ORCID,Kiltschewskij Dylan J.ORCID,Di Biase Maria A.,Gerring Zachary F.ORCID,Kundu KousikORCID,Surendran Praveen,Greco Laura A.ORCID,Clarke Erin D.ORCID,Collins Clare E.,Mondul Alison M.,Albanes Demetrius,Cairns Murray J.ORCID

Abstract

AbstractRetinol is a fat-soluble vitamin that plays an essential role in many biological processes throughout the human lifespan. Here, we perform the largest genome-wide association study (GWAS) of retinol to date in up to 22,274 participants. We identify eight common variant loci associated with retinol, as well as a rare-variant signal. An integrative gene prioritisation pipeline supports novel retinol-associated genes outside of the main retinol transport complex (RBP4:TTR) related to lipid biology, energy homoeostasis, and endocrine signalling. Genetic proxies of circulating retinol were then used to estimate causal relationships with almost 20,000 clinical phenotypes via a phenome-wide Mendelian randomisation study (MR-pheWAS). The MR-pheWAS suggests that retinol may exert causal effects on inflammation, adiposity, ocular measures, the microbiome, and MRI-derived brain phenotypes, amongst several others. Conversely, circulating retinol may be causally influenced by factors including lipids and serum creatinine. Finally, we demonstrate how a retinol polygenic score could identify individuals more likely to fall outside of the normative range of circulating retinol for a given age. In summary, this study provides a comprehensive evaluation of the genetics of circulating retinol, as well as revealing traits which should be prioritised for further investigation with respect to retinol related therapies or nutritional intervention.

Funder

Department of Health | National Health and Medical Research Council

Publisher

Springer Science and Business Media LLC

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