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胆汁酸的肠道吸收:14 kDa回肠脂质结合蛋白在差异光亲和标记中的矛盾行为。

Intestinal absorption of bile acids: paradoxical behaviour of the 14 kDa ileal lipid-binding protein in differential photoaffinity labelling.

作者信息

Kramer W, Corsiero D, Friedrich M, Girbig F, Stengelin S, Weyland C

机构信息

Research Metabolic Diseases, Hoechst Marion Roussel Deutschland GmbH, D-65926 Frankfurt am Main, Federal Republic of Germany.

出版信息

Biochem J. 1998 Jul 15;333 ( Pt 2)(Pt 2):335-41. doi: 10.1042/bj3330335.

Abstract

Photoaffinity labelling of brush border membrane vesicles from rabbit ileum with radiolabelled 3,3-azo and 7,7-azo derivatives of taurocholate identified integral membrane proteins of molecular masses 93 and 46 kDa, as well as a 14 kDa peripheral membrane protein, as components of the ileal Na+/bile acid transport system [Kramer, Girbig, Gutjahr, Kowalewski, Jouvenal, Müller, Tripier and Wess (1993) J. Biol. Chem. 268, 18035-18046]. Differential photoaffinity labelling in the presence of non-radiolabelled bile acid derivatives led, as expected, to a concentration-dependent decrease in the extent of labelling of the 93 and 46 kDa transmembrane proteins, which are the monomeric and dimeric forms of the ileal bile acid transporter protein. The extent of labelling of the 14 kDa ileal lipid-binding protein (ILBP), however, increased on the addition of unlabelled bile acids, the increase being dependent on the structure of the bile acid added. The possibility of artifacts was excluded by photoaffinity labelling experiments in the frozen state as well as by model calculations. The experimental results suggest that the binding of bile acids to ILBP can increase the affinity of ILBP for bile acids. These results would be in accordance with a substrate-load modification of transport activity and a positive-feedback regulation mechanism for active uptake of bile acid in the ileum.

摘要

用放射性标记的牛磺胆酸盐的3,3-偶氮和7,7-偶氮衍生物对兔回肠刷状缘膜囊泡进行光亲和标记,鉴定出分子量为93 kDa和46 kDa的整合膜蛋白以及一种14 kDa的外周膜蛋白,它们是回肠Na⁺/胆汁酸转运系统的组成成分[克莱默、吉尔比格、古特雅尔、科瓦列夫斯基、朱维纳尔、米勒、特里皮尔和韦斯(1993年)《生物化学杂志》268, 18035 - 18046]。在存在非放射性标记胆汁酸衍生物的情况下进行差异光亲和标记,正如预期的那样,导致93 kDa和46 kDa跨膜蛋白的标记程度呈浓度依赖性降低,这两种蛋白分别是回肠胆汁酸转运蛋白的单体和二聚体形式。然而,添加未标记胆汁酸后,14 kDa回肠脂质结合蛋白(ILBP)的标记程度增加,这种增加取决于所添加胆汁酸的结构。通过冷冻状态下的光亲和标记实验以及模型计算排除了假象的可能性。实验结果表明,胆汁酸与ILBP的结合可增加ILBP对胆汁酸的亲和力。这些结果与转运活性的底物负载调节以及回肠中胆汁酸主动摄取的正反馈调节机制相符。

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