Metabolomic analysis reveals vitamin D-induced decrease in polyol pathway and subtle modulation of glycolysis in HEK293T cells

GC Santos, JD Zeidler, JA Pérez-Valencia… - Scientific reports, 2017 - nature.com
GC Santos, JD Zeidler, JA Pérez-Valencia, ACB Sant'Anna-Silva, AT Da Poian, T El-Bacha
Scientific reports, 2017nature.com
We combined 1H NMR metabolomics with functional and molecular biochemical assays to
describe the metabolic changes elicited by vitamin D in HEK293T, an embryonic
proliferative cell line adapted to high-glucose concentrations. Activation of the polyol
pathway, was the most important consequence of cell exposure to high glucose
concentration, resembling cells exposed to hyperglycemia. Vitamin D induced alterations in
HEK293T cells metabolism, including a decrease in sorbitol, glycine, glutamate, guanine …
Abstract
We combined 1H NMR metabolomics with functional and molecular biochemical assays to describe the metabolic changes elicited by vitamin D in HEK293T, an embryonic proliferative cell line adapted to high-glucose concentrations. Activation of the polyol pathway, was the most important consequence of cell exposure to high glucose concentration, resembling cells exposed to hyperglycemia. Vitamin D induced alterations in HEK293T cells metabolism, including a decrease in sorbitol, glycine, glutamate, guanine. Vitamin D modulated glycolysis by increasing phosphoglycerate mutase and decreasing enolase activities, changing carbon fate without changing glucose consumption, lactate export and Krebs cycle. The decrease in sorbitol intracellular concentration seems to be related to vitamin D regulated redox homeostasis and protection against oxidative stress, and helped maintaining the high proliferative phenotype, supported by the decrease in glycine and guanine and orotate concentration and increase in choline and phosphocholine concentration. The decrease in orotate and guanine indicated an increased biosynthesis of purine and pyrimidines. Vitamin D elicited metabolic alteration without changing cellular proliferation and mitochondrial respiration, but reclaiming reductive power. Our study may contribute to the understanding of the metabolic mechanism of vitamin D upon exposure to hyperglycemia, suggesting a role of protection against oxidative stress.
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