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肝细胞中多特异性胆汁酸转运蛋白的新底物:某些线性肾素抑制肽对胆汁酸转运蛋白的干扰

New substrates of the multispecific bile acid transporter in liver cells: interference of some linear renin inhibiting peptides with transport protein(s) for bile acids.

作者信息

Bertrams A A, Ziegler K

机构信息

Institut für Pharmakologie und Toxikologie, Justus-Liebig-Universität Giessen, F.R.G.

出版信息

Biochim Biophys Acta. 1991 Jan 23;1073(1):213-20. doi: 10.1016/0304-4165(91)90205-u.

Abstract

Interactions between some stable linear peptides with renin inhibitory activity and a multispecific transport system in the basolateral plasma membrane of liver cells was studied on cell suspensions. The peptides used in our experiments were taken up by liver cells and subsequently eliminated without any biotransformation (e.g., proteolysis). No degradation products could be detected in the extracellular medium by thin-layer chromatography. All peptides tested inhibited the uptake of physiological and of some foreign substrates of the multispecific bile acid transporter (MT). The phalloidin response of liver cells was also inhibited to a similar degree in a concentration-dependent manner. The potency of inhibition did not correlate with the lipophilic properties of the peptides. On the other hand a tight correlation could be documented between the inhibition of cholate transport and that of the phalloidin response. Transport inhibition of typical substrates of the MT by the above renin inhibitors was competitive. In contrast, the transport of a typical substrate of the bilirubin carrier (rifampicin), of amino acids (alpha-aminoisobutyric acid), long chain fatty acids (oleic acid) and cationic compounds (thiamin hydrochloride) was not inhibited by the same renin inhibitors. These results indicate that linear renin inhibiting peptides are taken up into liver cells by carrier proteins related to the MT.

摘要

在细胞悬液上研究了一些具有肾素抑制活性的稳定线性肽与肝细胞基底外侧质膜中的多特异性转运系统之间的相互作用。我们实验中使用的肽被肝细胞摄取,随后未经任何生物转化(如蛋白水解)就被消除。通过薄层色谱法在细胞外培养基中未检测到降解产物。所有测试的肽都抑制了多特异性胆汁酸转运体(MT)的生理底物和一些外来底物的摄取。肝细胞对鬼笔环肽的反应也以浓度依赖的方式受到类似程度的抑制。抑制效力与肽的亲脂性无关。另一方面,可以证明胆酸盐转运的抑制与鬼笔环肽反应的抑制之间存在紧密的相关性。上述肾素抑制剂对MT典型底物的转运抑制是竞争性的。相反,胆红素载体的典型底物(利福平)、氨基酸(α-氨基异丁酸)、长链脂肪酸(油酸)和阳离子化合物(盐酸硫胺素)的转运不受相同肾素抑制剂的抑制。这些结果表明,线性肾素抑制肽通过与MT相关的载体蛋白被摄取到肝细胞中。

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