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首页> 外文期刊>American Journal of Physiology >Mechanism of inhibition of Na+-bile acid cotransport during chronic ileal inflammation in rabbits.
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Mechanism of inhibition of Na+-bile acid cotransport during chronic ileal inflammation in rabbits.

机译:兔慢性回肠炎症过程中Na +-胆汁酸共转运的抑制机制。

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In the chronically inflamed ileum, unique mechanisms of alteration of similar transport processes suggest regulation by different immune-inflammatory mediator pathways. In a rabbit model of chronic ileitis, we previously demonstrated that Na+-glucose cotransport was inhibited by a decrease in the cotransporter numbers, whereas Na+-amino acid cotransport was inhibited by a decrease in the affinity for the amino acid. In this study, we demonstrated that Na+-bile acid cotransport was reduced in villus cells from the chronically inflamed ileum. In villus cell brush-border membrane vesicles from the chronically inflamed ileum, Na+-bile acid cotransport was reduced as well, suggesting a direct effect at the cotransporter itself. Kinetic studies demonstrated that Na+-bile acid cotransport was inhibited by both a decrease in the affinity as well as a decrease in the maximal rate of uptake of the bile acid. Analysis of steady-state mRNA and immunoreactive protein levels of the Na+-bile acid cotransporter also demonstrated some reduction during chronic ileitis. Thus, in the chronically inflamed ileum, the mechanisms of inhibition of Na+-glucose, Na+-amino acid, and Na+-bile acid cotransport are different. These data suggest that different cotransporters are uniquely altered either secondary to their intrinsic differences or by different immune-inflammatory mediators during chronic ileitis.
机译:在慢性发炎的回肠中,相似的转运过程改变的独特机制提示通过不同的免疫-炎症介质途径进行调节。在慢性回肠炎的兔子模型中,我们先前证明了共转运蛋白数量的减少会抑制Na +-葡萄糖的共转运,而对氨基酸亲和力的降低会抑制Na +-氨基酸的共转运。在这项研究中,我们证明了在慢性发炎回肠的绒毛细胞中,Na +-胆汁酸的共转运减少了。在来自慢性发炎的回肠的绒毛细胞刷状边界膜囊泡中,Na +-胆汁酸的共转运也减少了,表明对共转运蛋白本身有直接作用。动力学研究表明,Na +-胆汁酸的共转运受到亲和力的降低以及胆汁酸最大摄取率的降低的抑制。对Na +-胆汁酸共转运蛋白的稳态mRNA和免疫反应蛋白水平的分析也显示出在慢性回肠炎期间某些减少。因此,在慢性发炎的回肠中,Na +-葡萄糖,Na +-氨基酸和Na +-胆汁酸共转运的抑制机制是不同的。这些数据表明,在慢性回肠炎期间,不同的共转运蛋白是继其固有差异之后或由于不同的免疫炎症介质而唯一改变的。

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