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首页> 外文期刊>Pfluegers Archiv: European Journal of Physiology >Efflux properties of basolateral peptide transporter in human intestinal cell line Caco-2.
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Efflux properties of basolateral peptide transporter in human intestinal cell line Caco-2.

机译:基底外侧肽转运蛋白在人肠道细胞系Caco-2中的外排特性。

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Small peptides and some pharmacologically active compounds are absorbed from the small intestine by the apical H(+)-coupled peptide transporter 1 (PEPT1) and the basolateral peptide transporter. Here we investigated the efflux properties of the basolateral peptide transporter in Caco-2 cells using two strategies, efflux measurements and a kinetic analysis of transepithelial transport of glycylsarcosine (Gly-Sar). [(14)C]Gly-Sar efflux through the basolateral membrane was not affected significantly by the external pH. Both approaches revealed that the basolateral peptide transporter was saturable in the efflux direction, and that the affinity was lower than that in the influx direction. For two peptide-like drugs, there was no difference in substrate recognition by the basolateral peptide transporter between the two sides of the membrane. Using the kinetic parameters of PEPT1 and the basolateral peptide transporter, a computational model of Gly-Sar transport in Caco-2 cells was constructed. The simulation fitted the experimental data well. Our findings suggested that substrate affinity of the basolateral peptide transporter is apparently asymmetric, but pH-dependence and substrate specificity are symmetric for the two directions of transport. The behaviour of Gly-Sar in Caco-2 cells could be predicted by a mathematical model describing the peptide transporters.
机译:小肽和一些药理活性化合物被顶端H(+)偶联肽转运蛋白1(PEPT1)和基底外侧肽转运蛋白从小肠吸收。在这里,我们使用两种策略,即流出测量和糖基肌氨酸(Gly-Sar)经上皮转运的动力学分析,研究了基底外侧肽转运蛋白在Caco-2细胞中的流出特性。 [(14)C] Gly-Sar通过基底外侧膜的外流不受外部pH值的显着影响。两种方法都表明基底外侧肽转运蛋白在外排方向上是可饱和的,并且亲和力比在流入方向上低。对于两种肽样药物,基底外侧肽转运蛋白在膜的两侧之间对底物的识别没有差异。利用PEPT1和基底外侧肽转运蛋白的动力学参数,构建了Caco-2细胞中Gly-Sar转运的计算模型。仿真结果很好地拟合了实验数据。我们的发现表明,基底外侧肽转运蛋白的底物亲和力显然是不对称的,但pH依赖性和底物特异性在两个运输方向上都是对称的。可以通过描述肽转运蛋白的数学模型预测Gly-Sar在Caco-2细胞中的行为。

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