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参与核糖体与糙面内质网结合的膜蛋白重构入脂质体。核糖体结合能力。

Reconstitution into liposomes of membrane proteins involved in ribosome binding on rough endoplasmic reticulum. Ribosome-binding capacity.

作者信息

Yamaguchi M, Sakai M, Horigome T, Omata S, Sugano H

出版信息

Biochem J. 1981 Mar 15;194(3):907-13. doi: 10.1042/bj1940907.

Abstract

A membrane protein fraction having a high affinity for polyribosomes was isolated from microsomal membranes of rat liver and was incorporated into liposomes made from microsomal lipids to evaluate the polyribosome-binding capacity of the reconstituted liposomes, with the following results. (1) The polyribosome binding to the reconstituted liposomes depended on the amounts of polyribosomes added to the binding mixture. (2) Liposomes made from lipids alone did not bind any polyribosomes. (3) The polyribosome-binding capacity of the reconstituted liposomes was very sensitive to proteolytic enzyme and strongly inhibited by addition of 0.1 mM-aurintricarboxylic acid or by increasing KCl concentration. These results suggest that the binding mechanism of polyribosomes to the reconstituted liposomes is much like that for rough microsomal membrane stripped of endogenous polyribosomes.

摘要

从大鼠肝脏微粒体膜中分离出一种对多核糖体具有高亲和力的膜蛋白组分,并将其整合到由微粒体脂质制成的脂质体中,以评估重构脂质体的多核糖体结合能力,结果如下:(1)多核糖体与重构脂质体的结合取决于添加到结合混合物中的多核糖体数量。(2)仅由脂质制成的脂质体不结合任何多核糖体。(3)重构脂质体的多核糖体结合能力对蛋白水解酶非常敏感,并被添加0.1 mM金精三羧酸或增加氯化钾浓度强烈抑制。这些结果表明,多核糖体与重构脂质体的结合机制与去除内源性多核糖体的糙面微粒体膜的结合机制非常相似。

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