首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >Rabbit small intestine does not contain an annexin II/caveolin 1 complex as a target for 2-azetidinone cholesterol absorption inhibitors
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Rabbit small intestine does not contain an annexin II/caveolin 1 complex as a target for 2-azetidinone cholesterol absorption inhibitors

机译:兔小肠不含膜联蛋白II / caveolin 1复合物作为2-氮杂环丁酮胆固醇吸收抑制剂的靶标

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Intestinal cholesterol absorption is specifically inhibited by the 2-azetidinone cholesterol absorption inhibitor ezetimibe. Photoreactive ezetimibe analogues specifically label a 145-kDa protein in the brush border membrane of enterocytes from rabbit small intestine identified as aminopeptidase N (CD13). In zebrafish and mouse small intestinal cytosol, a heterocomplex of M-r 52 kDa between annexin II and caveolin 1 was suggested as a target of ezetimibe. In contrast, in the cytosol and brush border membrane vesicles (BBMV) from rabbit small intestine of control animals or rabbits treated with the nonabsorbable cholesterol absorption inhibitor AVE 5530, both annexin II and caveolin 1 were exclusively present as monomers without any heterocomplex formation. Upon immunoprecipitation with annexin II a 52-kDa band was observed after immunostaining with annexin II antibodies, whereas no staining of a 52-kDa band occurred with anti-caveolin 1 antibodies. Vice versa, a 52-kDa band obtained by immunoprecipitation with caveolin 1 antibodies did not stain with annexin H-antibodies. The intensity of the 52-kDa band was dependent on the amount of antibody and was also observed with anti-actin or anti-APN antibodies suggesting that the 52-kDa band is a biochemical artefact. After incubation of cytosol or BBMV with radioactively labelled ezetimibe analogues, no significant amounts of the ezetimibe analogues could be detected in the immunoprecipitate with caveolin-1 or annexin II antibodies. Photoaffinity labelling of rabbit small intestinal BBMV with ezetimibe analogues did not result in labelling of proteins being immunoreactive with annexin II, caveolin 1 or a 52-kDa heterocomplex. These findings indicate that the rabbit small intestine does not contain an annexin II/caveolin 1 heterocomplex as a target for ezetimibe. (c) 2005 Elsevier B.V. All rights reserved.
机译:2-氮杂环丁酮胆固醇吸收抑制剂依泽替米贝可特异性抑制肠道胆固醇的吸收。光反应性依泽替米贝类似物在兔小肠肠细胞的刷状缘膜上特异性标记了一个145-kDa的蛋白质,被鉴定为氨基肽酶N(CD13)。在斑马鱼和小鼠小肠细胞质中,膜联蛋白II和小窝蛋白1之间的M-r 52 kDa杂合体被建议作为依泽替米贝的靶标。相反,在对照动物的兔子小肠或用不可吸收的胆固醇吸收抑制剂AVE 5530处理的兔子的小肠的胞液和刷状缘膜囊泡(BBMV)中,膜联蛋白II和小窝蛋白1均以单体形式存在,没有形成任何杂合物。用膜联蛋白II进行免疫沉淀后,用膜联蛋白II抗体免疫染色后观察到52 kDa的条带,而抗小孔蛋白1抗体未出现52 kDa的条带的染色。反之亦然,通过用小窝蛋白1抗体免疫沉淀获得的52 kDa条带未被膜联蛋白H抗体染色。 52 kDa条带的强度取决于抗体的量,还可以用抗肌动蛋白或抗APN抗体观察到,表明52 kDa条带是一种生化制品。将细胞溶质或BBMV与放射性标记的ezetimibe类似物孵育后,用Caveolin-1或膜联蛋白II抗体在免疫沉淀物中未检测到大量的ezetimibe类似物。用依泽替米贝类似物对兔小肠BBMV进行光亲和性标记不会导致与膜联蛋白II,小窝蛋白1或52 kDa异源复合物具有免疫反应性的蛋白质标记。这些发现表明,兔子小肠不包含膜联蛋白II / caveolin 1杂合物作为依泽替米贝的靶标。 (c)2005 Elsevier B.V.保留所有权利。

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