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Differential expression of cholangiocyte and ileal bile acid transporters following bile acid supplementation and depletion

机译:补充和清除胆汁酸后胆管细胞和回肠胆汁酸转运蛋白的差异表达

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AIM: We have previously demonstrated that cholangiocytes, the epithelial cells lining intrahepatic bile ducts, encode two functional bile acid transporters via alternative splicing of a single gene to facilitate bile acid vectorial transport. Cholangiocytes possess ASBT, an apical sodium-dependent bile acid transporter to take up bile acids, and t-ASBT, a basolateral alternatively spliced and truncated form of ASBT to efflux bile acids. Though hepatocyte and ileal bile acid transporters are in part regulated by the flux of bile acids, the effect of alterations in bile acid flux on the expression of t-ASBT in terminal ileocytes remains unclear. Thus, we tested the hypothesis that expression of ASBT and t-ASBT in cholangiocytes and ileocytes was regulated by bile acid flux. METHODS: Expression of ASBT and t-ASBT message and protein in cholangiocytes and ileocytes isolated from pair-fed rats given control (C) and 1% taurocholate (TCA) or 5% cholestyramine (CY) enriched diets, were assessed by both quantitative RNase protection assays and quantitative immunoblotting. The data obtained from each of the control groups were pooled to reflect the changes observed following TCA and CY treatments with respect to the control diets. Cholangiocyte taurocholate uptake was determined using a novel microperfusion technique on intrahepatic bile duct units (IBDUs) derived from C, TCA and CY fed rats. RESULTS: In cholangiocytes, both ASBT and t-ASBT message RNA and protein were significantly decreased in response to TCA feeding compared to C diet. In contrast, message and protein of both bile acid transporters significantly increased following CY feeding compared to C diet. In the ileum, TCA feeding significantly up-regulated both ASBT and t-ASBT message and protein compared to C diet, while CY feeding significantly down-regulated message and protein of both bile acid transporters compared to C diet. As anticipated from alterations in cholangiocyte ASBT expression, the uptake of taurocholate in microperfused IBDUs derived from rats on TCA diet decreased 2.7-fold, whereas it increased 1.7-fold in those on CY diet compared to C diet fed groups. CONCLUSION: These data demonstrate that expression of ASBT and t-ASBT in cholangiocytes is regulated by a negative feedback loop while the expression of these transporters in terminal ileum is modified via positive feedback. Thus, while transcriptional regulatory mechanisms in response to alterations in bile acid pool size are operative in both cholangiocytes and ileocytes, each cell type responds differently to bile acid supplementation and depletion.
机译:目的:我们以前已经证明胆管细胞,即肝内胆管内衬的上皮细胞,通过单个基因的可变剪接编码两种功能性胆汁酸转运蛋白,以促进胆汁酸矢量转运。胆管细胞拥有ASBT(一种顶端钠依赖性胆汁酸转运蛋白,可吸收胆汁酸)和t-ASBT(一种基底外侧交替剪接和截短形式的ASBT来排出胆汁酸)。尽管肝细胞和回肠胆汁酸转运蛋白部分受胆汁酸流量调节,但胆汁酸流量变化对终末回肠细胞t-ASBT表达的影响尚不清楚。因此,我们测试了胆汁酸通量调节胆管细胞和回肠细胞中ASBT和t-ASBT表达的假设。方法:通过定量RNase评估了从成对喂养的大鼠中分离的胆汁细胞和回肠细胞中ASBT,t-ASBT信息和蛋白的表达,并给予了1%牛磺胆酸盐(TCA)或5%胆甾胺(CY)的饮食。保护测定和定量免疫印迹。汇总从每个对照组获得的数据,以反映在TCA和CY处理后相对于对照饮食观察到的变化。使用新型微灌流技术对源自C,TCA和CY喂养的大鼠的肝内胆管单位(IBDU)进行测定,测定胆管细胞牛磺胆酸盐的摄取量。结果:与C日粮相比,TCA喂养可显着降低胆管细胞的ASBT和t-ASBT信息RNA和蛋白质。相反,与C日粮相比,CY饲喂后两种胆汁酸转运蛋白的信息和蛋白质均显着增加。在回肠中,与C日粮相比,TCA喂养显着上调了ASBT和t-ASBT信息和蛋白质,而CY日粮显着下调了两种胆汁酸转运蛋白的信息和蛋白质。正如从胆管细胞ASBT表达的变化所预期的那样,与C日粮组相比,TCA日粮的大鼠微灌流IBDU中牛磺胆酸盐的摄取减少了2.7倍,而CY日粮中的牛磺胆碱的摄取增加了1.7倍。结论:这些数据表明胆管细胞中ASBT和t-ASBT的表达受到负反馈环的调节,而回肠末端这些转运蛋白的表达则通过正反馈被修饰。因此,尽管响应胆汁酸池大小改变的转录调控机制在胆管细胞和回肠细胞中均有效,但每种细胞类型对胆汁酸补充和耗竭的反应不同。

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