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ATP-dependent transport of organic anions into isolated basolateral membrane vesicles from rat intestine.

机译:ATP依赖的有机阴离子从大鼠肠道进入离体的基底外侧膜囊泡的运输。

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摘要

The mechanism for the cellular extrusion of organic anions across the intestinal basolateral membrane was examined using isolated membrane vesicles from rat jejunum, ileum, and colon. It was found that 17beta-estradiol 17beta-D-glucuronide (E217betaG) is taken up in an ATP-dependent manner into the basolateral membrane vesicles (BLMVs) but not into the brush-border or microsomal counterparts. The ATP-dependent uptake of E217betaG into BLMVs from jejunum and ileum was described by a single component with a Km value of 23.5 and 8.31 microM, respectively, whereas that into the BLMVs from colon was described by assuming the presence of high (Km=0.82 microM)- and low-affinity (Km=35.4 microM) components. Taurocholate, 6-hydroxy-5,7-dimethyl-2-methylamino-4-(3-pyridylmethyl) benzothiazole glucuronide and taurolithocholate sulfate, but not leukotriene C4, were significantly taken up by the BLMVs. In addition to such substrate specificity, the inhibitor sensitivity of the ATP-dependent transport in BLMVs was similar to that of rat multidrug resistance-associated protein 3 (Mrp3), which is located on the basolateral membrane of enterocytes. Together with the fact that the rank order of the extent of the expression of Mrp3 (jejunum < ileum colon) is in parallel with that of the extent of the transport of ligands, these results suggest that the ATP-dependent uptake of organic anions into isolated intestinal BLMVs is at least partly mediated by Mrp3.
机译:使用来自大鼠空肠,回肠和结肠的分离的膜囊泡,检查了有机阴离子穿过肠基底外侧膜的细胞挤出机制。发现17beta-雌二醇17beta-D-葡萄糖醛酸(E217betaG)以ATP依赖的方式被吸收到基底外侧膜囊泡(BLMVs)中,但不吸收到刷状边界或微粒体对应物中。空腹和回肠的BLMV中E217betaG的ATP依赖性吸收分别由Km值为23.5和8.31 microM的单个成分描述,而结肠中的E217betaG假定存在高(Km = 0.82 microM)和低亲和力(Km = 35.4 microM)组件。 BLMV显着吸收了牛磺胆酸盐,6-羟基-5,7-二甲基-2-甲基氨基-4-(3-吡啶基甲基)苯并噻唑葡糖醛酸和牛磺石胆酸盐硫酸盐,但不吸收白三烯C4。除了这种底物特异性外,BLMV中ATP依赖性转运的抑制剂敏感性与大鼠多药耐药性相关蛋白3(Mrp3)相似,后者位于肠上皮细胞的基底外侧膜上。再加上Mrp3(空肠<回肠<结肠)的表达范围与配体运输的范围平行,这些结果表明,ATP依赖于有机阴离子的吸收分离的肠BLMV中至少部分地由Mrp3介导。

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