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Differentiation-dependent regulation of intestinal vitamin B2 uptake: studies utilizing human-derived intestinal epithelial Caco-2 cells and native rat intestine

机译:肠道维生素B2摄取的差异依赖性调节:利用人源性肠上皮Caco-2细胞和天然大鼠肠的研究

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摘要

Intestinal epithelial cells undergo differentiation as they move from the crypt to the villi, a process that is associated with up- and downregulation in expression of a variety of genes, including those involved in nutrient absorption. Whether the intestinal uptake process of vitamin B2 [riboflavin (RF)] also undergoes differentiation-dependent regulation and the mechanism through which this occurs are not known. We used human-derived intestinal epithelial Caco-2 cells and native rat intestine as models to address these issues. Caco-2 cells showed a significantly higher carrier-mediated RF uptake in post- than preconfluent cells. This upregulation was associated with a significantly higher level of protein and mRNA expression of the RF transporters hRFVT-1 and hRFVT-3 in the post- than preconfluent cells; it was also accompanied with a significantly higher rate of transcription of the respective genes (SLC52A1 and SLC52A3), as indicated by the higher level of expression of heterogeneous nuclear RNA and higher promoter activity in post- than preconfluent cells. Studies with native rat intestine also showed a significantly higher RF uptake by epithelial cells of the villus tip than epithelial cells of the crypt; this again was accompanied by a significantly higher level of expression of the rat RFVT-1 and RFVT-3 at the protein, mRNA, and heterogeneous nuclear RNA levels. These findings show, for the first time, that the intestinal RF uptake process undergoes differentiation-dependent upregulation and suggest that this is mediated (at least in part) via transcriptional mechanisms.
机译:肠道上皮细胞在从隐窝移动到绒毛时会经历分化,这一过程与多种基因表达的上调和下调有关,包括参与营养吸收的基因。维生素B2 [核黄素(RF)]的肠道摄取过程是否也经历了分化依赖性调节,其发生机理尚不清楚。我们使用人类来源的肠上皮Caco-2细胞和天然大鼠肠作为模型来解决这些问题。 Caco-2细胞在融合后的细胞中显示出明显更高的载体介导的RF摄取。这种上调与融合后的细胞中RF转运蛋白hRFVT-1和hRFVT-3的蛋白和mRNA表达水平显着相关。它也伴随着相应基因(SLC52A1和SLC52A3)的显着更高的转录速率,这表明,与融合前相比,异质核RNA的表达水平更高,启动子活性更高。对天然大鼠肠道的研究还显示,绒毛尖端的上皮细胞的RF摄取要比隐窝的上皮细胞高得多。这再次伴随着大鼠RFVT-1和RFVT-3在蛋白质,mRNA和异质核RNA水平的表达水平显着升高。这些发现首次表明,肠道RF吸收过程经历了分化依赖性上调,并表明这是(至少部分地)通过转录机制介导的。

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