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单羧酸转运蛋白MCT1介导的弱有机酸pH依赖性肠道吸收的免疫组织化学和功能特性

Immunohistochemical and functional characterization of pH-dependent intestinal absorption of weak organic acids by the monocarboxylic acid transporter MCT1.

作者信息

Tamai I, Sai Y, Ono A, Kido Y, Yabuuchi H, Takanaga H, Satoh E, Ogihara T, Amano O, Izeki S, Tsuji A

机构信息

Faculty of Pharmaceutical Sciences, Kanazawa University, Japan.

出版信息

J Pharm Pharmacol. 1999 Oct;51(10):1113-21. doi: 10.1211/0022357991776804.

DOI:10.1211/0022357991776804
PMID:10579682
Abstract

The participation of the monocarboxylic acid transporter MCT1 in the intestinal absorption of weak organic acids has been clarified by functional characterization, by use of stably transfected cells, and by immunohistochemical location of the transporter in intestinal tissues. Immunohistochemical analysis by use of the anti-MCT1 antibody showed that MCT1 is distributed throughout the upper and lower intestines, especially in the basolateral membrane and, to a lesser extent, in the brush-border membrane. When the transporter gene rat MCT1 was transfected into MDA-MB231 cells, transport of benzoic acid, a model weak organic acid that has been generally believed to be transported across the cell membranes by passive diffusion, and lactic acid in rat MCT1-transfected cells was significantly increased compared with transport in cells transfected with the expression vector pRc-CMV alone (mock cells). The observed transport was pH-dependent and activity increased between pH 7.5 and pH 5.5, whereas pH-dependence in mock cells was moderate. Rat MCT1-mediated benzoic acid uptake was saturable, with an apparent Km value of 3.05 mM. In addition, MCT1 increased the efflux of [14C]benzoic acid from the cells. Several weak organic acids were also transported by rat MCT1. These results show that pH-dependent intestinal absorption of weak organic acids, previously explained in terms of passive diffusion according to the pH-partition hypothesis, is at least partially accounted for by MCT1-mediated transport energized at acidic pH by utilization of the proton gradient as a driving force.

摘要

单羧酸转运蛋白MCT1在肠道对弱有机酸的吸收中的作用,已通过功能特性鉴定、利用稳定转染细胞以及通过该转运蛋白在肠道组织中的免疫组化定位得以阐明。使用抗MCT1抗体进行的免疫组化分析表明,MCT1分布于整个小肠和大肠,尤其在基底外侧膜,在刷状缘膜中的分布较少。当将转运蛋白基因大鼠MCT1转染至MDA-MB231细胞时,与仅用表达载体pRc-CMV转染的细胞(空载体细胞)相比,大鼠MCT1转染细胞中苯甲酸(一种通常被认为通过被动扩散跨细胞膜转运的典型弱有机酸)和乳酸的转运显著增加。观察到的转运呈pH依赖性,在pH 7.5至pH 5.5之间活性增加,而空载体细胞中的pH依赖性则较弱。大鼠MCT1介导的苯甲酸摄取具有饱和性,表观Km值为3.05 mM。此外,MCT1增加了细胞中[14C]苯甲酸的外流。几种弱有机酸也可被大鼠MCT1转运。这些结果表明,先前根据pH分配假说用被动扩散解释的弱有机酸的pH依赖性肠道吸收,至少部分是由MCT1介导的转运所引起的,该转运在酸性pH条件下利用质子梯度作为驱动力来提供能量。

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