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人肠上皮细胞(Caco-2)中二肽/三肽转运体的底物特异性:对经历H⁺偶联吸收的底物的鉴定。

Substrate specificity of the di/tripeptide transporter in human intestinal epithelia (Caco-2): identification of substrates that undergo H(+)-coupled absorption.

作者信息

Thwaites D T, Hirst B H, Simmons N L

机构信息

Department of Physiological Sciences, University of Newcastle upon Tyne, Medical School.

出版信息

Br J Pharmacol. 1994 Nov;113(3):1050-6. doi: 10.1111/j.1476-5381.1994.tb17099.x.

Abstract
  1. pH-dependent transepithelial transport and intracellular accumulation of the hydrolysis-resistant dipeptide glycylsarcosine (Gly-Sar) have been demonstrated in the model human intestinal epithelial cell line, Caco-2. 2. Experiments with BCECF (2',7'-bis(2-carboxyethyl)-5(6)-carboxyfluorescein)-loaded Caco-2 cells demonstrated that dipeptide (Gly-Sar) transport across the apical membrane is coupled to proton flow into the cell. 3. A range of postulated substrates for the intestinal di/tripeptide carrier were tested for their abilities to: (a) inhibit pH-dependent [14C]Gly-Sar apical-to-basal transport and intracellular accumulation and (b) stimulate H+ flow across the apical surface of BCECF-loaded Caco-2 cell monolayers. 4. A range of compounds (including Gly-Gly, Leu-Leu, Gly-Gly-Gly, cefadroxil and cephalexin) caused marked acidification of intracellular pH when perfused at the apical surface of Caco-2 cell monolayers. In contrast leucine and D-Leu-D-Leu failed to induce proton flow. The ability to induce proton-flow across the apical surface by these compounds, in this intestinal epithelium, was directly correlated to the relative inhibitory effects on [14C]-Gly-Sar transport and accumulation. 5. The determination of substrate-induced intracellular pH change in the Caco-2 cell system may provide a useful rapid screen for candidate substrates for absorption via H(+)-coupled transport mechanisms such as the intestinal di/tripeptide carrier in an appropriate physiological context.
摘要
  1. 在人肠道上皮细胞系Caco-2模型中已证实,耐水解二肽甘氨酰肌氨酸(Gly-Sar)的跨上皮转运和细胞内积累具有pH依赖性。2. 对负载BCECF(2',7'-双(2-羧乙基)-5(6)-羧基荧光素)的Caco-2细胞进行的实验表明,二肽(Gly-Sar)跨顶端膜的转运与质子流入细胞相关联。3. 测试了一系列假定的肠道二肽/三肽载体底物的以下能力:(a)抑制pH依赖性的[14C]Gly-Sar从顶端到基底的转运和细胞内积累,以及(b)刺激质子流过负载BCECF的Caco-2细胞单层的顶端表面。4. 一系列化合物(包括甘氨酰甘氨酸、亮氨酰亮氨酸、甘氨酰甘氨酰甘氨酸、头孢羟氨苄和头孢氨苄)在灌注到Caco-2细胞单层的顶端表面时,会导致细胞内pH显著酸化。相比之下,亮氨酸和D-亮氨酰-D-亮氨酸未能诱导质子流动。在这种肠道上皮中,这些化合物诱导质子流过顶端表面的能力与对[14C]-Gly-Sar转运和积累的相对抑制作用直接相关。5. 在Caco-2细胞系统中测定底物诱导的细胞内pH变化,可能为通过H(+)偶联转运机制(如肠道二肽/三肽载体)吸收的候选底物提供一种有用的快速筛选方法,且处于适当的生理环境中。

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