The Role of Polymorphisms in Vitamin D-Related Genes in Response to Vitamin D Supplementation

Sara Tomei; Parul Singh; Rebecca Mathew; Valentina Mattei; Mathieu Garand; Mariam Alwakeel; Elham Sharif; Souhaila Al Khodor

doi:10.3390/nu12092608

The Role of Polymorphisms in Vitamin D-Related Genes in Response to Vitamin D Supplementation

Nutrients. 2020 Aug 27;12(9):2608. doi: 10.3390/nu12092608.

Authors

Sara Tomei¹, Parul Singh¹, Rebecca Mathew¹, Valentina Mattei¹, Mathieu Garand¹, Mariam Alwakeel², Elham Sharif², Souhaila Al Khodor¹

Affiliations

¹ Research Department, Sidra Medicine, Doha 26999, Qatar.
² Department of Biomedical Sciences, College of Health Sciences, Qatar University, Doha 26999, Qatar.

Abstract

Background: Vitamin D deficiency represents a major healthcare problem. Vitamin D status is influenced by genetic and environmental determinants. Several observational studies have evaluated the association of single-nucleotide polymorphisms (SNPs) in vitamin D-related genes and vitamin D levels. Nevertheless, little is known about the role of these SNPs in the response to vitamin D supplementation. We conducted an interventional study to define the association between SNPs in vitamin D-related genes and the response to vitamin D supplementation in 100 self-reported healthy women of Arab ancestry for the majority.

Methods: A total of 100 healthy female subjects received a weekly oral dose of 50,000 IU vitamin D for 12 weeks. Serum vitamin D concentration and metabolic profiles were measured at baseline and 12 weeks post-vitamin D supplementation. The genotypes of 37 SNPs selected from previously reported vitamin D-related genes have been assessed by Fluidigm genotyping assay.

Results: Rs731236 (VDR gene) and rs7116978 (CYP2R1 gene) showed a significant association with vitamin D status. The rs731236 GG genotype and the rs7116978 CC genotype were associated with a "vitamin D sufficiency" state. Rs731236 GG and rs7116978 CC genotypes showed a higher response to vitamin D supplementation. Transcription factor binding site prediction analysis showed altered binding sites for transcription factors according to the different rs7116978 alleles. Interestingly, the 37 SNPs previously established to play a role in vitamin D-related pathways explained very little of the response to vitamin D supplementation in our cohort, suggesting the existence of alternative loci whose number and effect size need to be investigated in future studies.

Conclusion: In this paper, we present novel data on vitamin D-related SNPs and response to vitamin D supplementation demonstrating the feasibility of applying functional genomic approaches in interventional studies to assess individual-level responses to vitamin D supplementation.

Keywords: 25(OH)D; 25-hydroxyvitamin D; SNP; blood; polymorphisms; single-nucleotide polymorphism; vitamin D; vitamin D deficiency.

MeSH terms

Adult
Arabs
Dietary Supplements*
Female
Follow-Up Studies
Humans
Polymorphism, Single Nucleotide / genetics*
Vitamin D / administration & dosage*
Vitamin D / blood
Vitamin D / genetics*
Vitamins / administration & dosage*
Vitamins / blood
Vitamins / genetics*
Young Adult

Substances

Vitamins
Vitamin D