Vitamin A Deficiency Clinical Trial
Official title:
Effect of SNPs in the Beta-carotene 15, 15'-Monooxygenase (BCMO1) Enzyme on Retinol Formation and Beta-carotene Plasma Responses
Summary:
Chronic intake of foods low in vitamin A (retinol) and provitamin A forming an unbalanced
diet with little variety is common in young individuals in the United Kingdom (UK)
population and can lead to subclinical micronutrient deficiency. Provitamin A sources such
as β-carotene are cleaved centrally by the β-carotene 15,15'-monooxygenase (BCMO1) into
retinal, the precursor of retinol. However, the amount of β-carotene and retinol produced
after ingestion of β-carotene is highly variable between healthy individuals, with
approximately 40% of the subjects being classified as low responders. Several stable isotope
studies have shown a large disparity between the most efficient converters and the most
inefficient converters of β-carotene with variations of up to 8-fold. It is possible that
differences in β-carotene response may be due to single nucleotide polymorphisms (SNPs) in
genes involved in aspects of β-carotene conversion. Previous work has shown that carriers of
both, the 379V and 267S+379V BCMO1 variant alleles had a reduced ability to convert
β-carotene. More importantly, 44% of the western population have the 379V haplotype. A high
percentage of the Western population may therefore not be able to achieve adequate vitamin A
intake if dietary β-carotene is a major source of their vitamin A intake. This is of
particular relevance to vegetarians, to young individuals aged 19-24 years who have lower
intakes of preformed retinol than any other age group, and to pregnant women. The aim of
this study is to establish whether the maximum recommended dose for β-carotene of 7mg/day by
the British Expert Committee on Vitamins and Minerals (EVM) can overcome the SNP effect in
the BCMO1 enzyme.
Hypothesis:
The investigators hypothesize that the current maximum recommended intake of 7 mg of
β-carotene per day cannot overcome the low convertor phenotype in BCMO1 to fulfill vitamin A
requirements in these people.
n/a
Allocation: Randomized, Endpoint Classification: Pharmacokinetics Study, Intervention Model: Parallel Assignment, Masking: Single Blind (Subject), Primary Purpose: Basic Science
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