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叶酸缺乏改变了雄性小鼠脂肪酸代谢、DNA 合成和昼夜节律的基因表达。

Folate depletion changes gene expression of fatty acid metabolism, DNA synthesis, and circadian cycle in male mice.

机构信息

INSERM U1028, CNRS UMR5292, Université Lyon 1, Centre de Recherche en Neurosciences, Neurooncologie et Neuroinflammation, Fac Med Laennec, F-69372 Lyon, Cedex 08, France.

出版信息

Nutr Res. 2012 Feb;32(2):124-32. doi: 10.1016/j.nutres.2011.12.012.

Abstract

Folate is essential for purine and thymidylate biosynthesis and in methyl transfer for DNA methylation. Folate deficiency alters the secretion of melatonin, a hormone involved in circadian rhythm entrainment, and causes hyperhomocysteinemia because of disruption of homocysteine metabolism. Adverse effects of homocysteine include the generation of free radicals, activation of proliferation or apoptosis, and alteration of gene expression. The liver is an important organ for folate metabolism, and its genome analysis has revealed numerous clock-regulated genes. The variations at the level of their expression during folate deficiency are not known. The aim of our study was to investigate the effects of folate deficiency on gene expression in the mouse liver. A control group receiving a synthetic diet and a folate-depleted group were housed for 4 weeks on a 12-hour/12-hour light/dark cycle. Three mice from each group were euthanized under dim red light at the beginning of the light cycle, and 3, at the beginning of the dark period. Gene expression was studied in a microarray analysis. Of the 53 genes showing modified daily expression in the controls, 52 showed a less marked or no difference after folate depletion. Only 1, lpin1, showed a more marked difference. Ten genes coding for proteins involved in lipid metabolism did not show a morning/evening difference in controls but did after folate depletion. This study shows that, in the mouse liver, dietary folate depletion leads to major changes in expression of several genes involved in fatty acid metabolism, DNA synthesis, and expression of circadian genes.

摘要

叶酸对于嘌呤和胸苷酸的生物合成以及 DNA 甲基化中的甲基转移至关重要。叶酸缺乏会改变褪黑素的分泌,褪黑素是一种参与昼夜节律同步的激素,并导致高同型半胱氨酸血症,因为同型半胱氨酸代谢受到干扰。同型半胱氨酸的不良反应包括自由基的产生、增殖或凋亡的激活以及基因表达的改变。肝脏是叶酸代谢的重要器官,其基因组分析揭示了许多时钟调节基因。在叶酸缺乏期间,其表达水平的变化尚不清楚。我们的研究目的是研究叶酸缺乏对小鼠肝脏基因表达的影响。一组接受合成饮食的对照组和一组叶酸缺乏组在 12 小时/12 小时光照/黑暗周期下饲养了 4 周。每组有 3 只小鼠在光照周期开始时在暗光下安乐死,有 3 只在黑暗期开始时安乐死。通过微阵列分析研究基因表达。在对照组中,53 个显示出每日表达改变的基因中,有 52 个在叶酸缺乏后显示出不太明显或没有差异。只有 1 个基因,即 lpin1,显示出更明显的差异。编码参与脂质代谢的蛋白质的 10 个基因在对照组中没有表现出早晚差异,但在叶酸缺乏后表现出差异。这项研究表明,在小鼠肝脏中,饮食中叶酸的缺乏会导致参与脂肪酸代谢、DNA 合成和昼夜节律基因表达的几个基因的表达发生重大变化。

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