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首页> 外文期刊>The Journal of Nutritional Biochemistry >Vitamin E decreases endogenous cholesterol synthesis and apo-AI-mediated cholesterol secretion in Caco-2 cells.
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Vitamin E decreases endogenous cholesterol synthesis and apo-AI-mediated cholesterol secretion in Caco-2 cells.

机译:维生素E减少Caco-2细胞中的内源性胆固醇合成和apo-AI介导的胆固醇分泌。

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Intestine is the gateway for newly absorbed tocopherols. This organ also plays a crucial role in cholesterol metabolism. Because tocopherols are known to impact cholesterol metabolism in the liver, we hypothesized that tocopherols could also modulate cholesterol metabolism in the intestine. This study aimed to verify this hypothesis and to unveil the mechanisms involved, using Caco-2 cells as a model of the human intestinal cell. Both alpha- and gamma-tocopherol significantly (P<.05) decreased endogenous cholesterol synthesis and apo-AI-mediated cholesterol secretion in Caco-2 cells. Tocopherols down-regulated (P<.05) up to half of the genes involved in the cholesterol synthesis pathway, together with CYP27A1, which is involved in oxysterol production. The activity of this enzyme, as well as the levels of intracellular oxysterols, was significantly diminished by tocopherols. Finally, tocopherols significantly reduced ABCA1 mRNA levels in Caco-2 cells. We conclude that tocopherols impair the endogenous synthesis and apo-AI-mediated secretion of cholesterol in Caco-2 cells. This effect involves a down-regulation of genes involved in the cholesterol synthesis pathway, resulting in down-regulation of CYP27A1 which, in turn, diminishes oxysterol concentrations. The outcome is a decrease of LXR activity, resulting in down-regulation of ABCA1. These data reinforce the effect of alpha- and gamma-tocopherol on cholesterol metabolism via gene expression regulation.
机译:肠是新吸收的生育酚的门户。该器官在胆固醇代谢中也起着至关重要的作用。因为已知生育酚会影响肝脏中的胆固醇代谢,所以我们假设生育酚也可以调节肠道中的胆固醇代谢。这项研究旨在验证这一假设并揭示涉及的机制,使用Caco-2细胞作为人肠道细胞的模型。 α-和γ-生育酚均显着(P <.05)降低了Caco-2细胞中的内源性胆固醇合成和apo-AI介导的胆固醇分泌。生育酚与CYP27A1一起下调与胆固醇合成途径有关的基因的一半(P <.05),而CYP27A1参与氧化胆固醇的产生。生育酚显着降低了该酶的活性以及细胞内氧固醇的水平。最后,生育酚显着降低了Caco-2细胞中ABCA1 mRNA的水平。我们得出的结论是,生育酚会损害Caco-2细胞中内源性合成和apo-AI介导的胆固醇分泌。该作用涉及胆固醇合成途径中涉及的基因的下调,导致CYP27A1的下调,进而降低了氧固醇的浓度。结果是LXR活性降低,导致ABCA1下调。这些数据通过基因表达调控增强了α-和γ-生育酚对胆固醇代谢的作用。

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