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外被体蛋白与氨基糖苷类抗生素的相互作用:外被体蛋白至少有两个双赖氨酸结合位点的证据。

Interaction of coatomer with aminoglycoside antibiotics: evidence that coatomer has at least two dilysine binding sites.

作者信息

Hudson R T, Draper R K

机构信息

Molecular and Cell Biology Program, University of Texas at Dallas, Richardson 75083-0688, USA.

出版信息

Mol Biol Cell. 1997 Oct;8(10):1901-10. doi: 10.1091/mbc.8.10.1901.

Abstract

Coatomer is the soluble precursor of the COPI coat (coat protein I) involved in traffic among membranes of the endoplasmic reticulum and the Golgi apparatus. We report herein that neomycin precipitates coatomer from cell extracts and from purified coatomer preparations. Precipitation first increased and then decreased as the neomycin concentration increased, analogous to the precipitation of a polyvalent antigen by divalent antibodies. This suggested that neomycin cross-linked coatomer into large aggregates and implies that coatomer has two or more binding sites for neomycin. A variety of other aminoglycoside antibiotics precipitated coatomer, or if they did not precipitate, they interfered with the ability of neomycin to precipitate. Coatomer is know to interact with a motif (KKXX) containing adjacent lysine residues at the carboxyl terminus of the cytoplasmic domains of some membrane proteins resident in the endoplasmic reticulum. All of the antibiotics that interacted with coatomer contain at least two close amino groups, suggesting that the antibiotics might be interacting with the di-lysine binding site of coatomer. Consistent with this idea, di-lysine itself blocked the interaction of antibiotics with coatomer. Moreover, di-lysine and antibiotics each blocked the coating of Golgi membranes by coatomer. These data suggest that certain aminoglycoside antibiotics interact with di-lysine binding sites on coatomer and that coatomer contains at least two of these di-lysine binding sites.

摘要

包被蛋白复合物是参与内质网和高尔基体膜间运输的COPI被膜(被膜蛋白I)的可溶性前体。我们在此报告,新霉素可从细胞提取物和纯化的包被蛋白复合物制剂中沉淀出包被蛋白复合物。随着新霉素浓度的增加,沉淀先增加后减少,这与二价抗体沉淀多价抗原的情况类似。这表明新霉素将包被蛋白复合物交联成大聚集体,意味着包被蛋白复合物有两个或更多新霉素结合位点。多种其他氨基糖苷类抗生素可沉淀包被蛋白复合物,或者如果它们不沉淀,则会干扰新霉素沉淀的能力。已知包被蛋白复合物与内质网中一些驻留膜蛋白细胞质结构域羧基末端含相邻赖氨酸残基的基序(KKXX)相互作用。所有与包被蛋白复合物相互作用的抗生素都至少含有两个相邻氨基,这表明抗生素可能与包被蛋白复合物的双赖氨酸结合位点相互作用。与此观点一致,双赖氨酸本身可阻断抗生素与包被蛋白复合物的相互作用。此外,双赖氨酸和抗生素均可阻断包被蛋白复合物对高尔基体膜的包被。这些数据表明某些氨基糖苷类抗生素与包被蛋白复合物上的双赖氨酸结合位点相互作用,且包被蛋白复合物至少含有两个此类双赖氨酸结合位点。

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