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多胺对蛋白激酶C与膜结合的抑制作用。

Inhibitory action of polyamines on protein kinase C association to membranes.

作者信息

Moruzzi M, Barbiroli B, Monti M G, Tadolini B, Hakim G, Mezzetti G

机构信息

Istituto di Chimica Biologica, Università di Modena, Italy.

出版信息

Biochem J. 1987 Oct 1;247(1):175-80. doi: 10.1042/bj2470175.

Abstract

Physiological activation of protein kinase C requires the interaction of this enzyme with cellular membranes [Nishizuka (1986) Science 233, 305-312]. In the present work a reconstituted system of protein kinase C and human inside-out erythrocyte vesicles was utilized to study the effect in vitro of naturally occurring polyamines on the activation process of protein kinase C. The active membrane-associated complex was conveniently determined by its ability to bind radioactive phorbol ester with an exact 1:1 stoichiometry. The association reaction of the enzyme to membrane was rapid, being complete within 1 min at 25 degrees C. The addition of polyamines, particularly spermine, greatly decreased in a dose-dependent manner the amount of protein kinase C bound to membranes (i.e. in the activated form). The effect observed was quite specific, since it was dependent on the chemical structure of the polyamine and it was manifest at micromolar concentrations of the polycation; the order of potency was spermine greater than spermidine greater than putrescine. A characterization of this effect is presented and possible physiological implications are discussed.

摘要

蛋白激酶C的生理激活需要该酶与细胞膜相互作用[西冢(1986年)《科学》233卷,305 - 312页]。在本研究中,利用蛋白激酶C与人内翻红细胞囊泡的重构系统,来研究天然存在的多胺在体外对蛋白激酶C激活过程的影响。通过活性膜相关复合物以精确的1:1化学计量比结合放射性佛波酯的能力,可方便地对其进行测定。该酶与膜的结合反应迅速,在25℃下1分钟内即可完成。多胺的加入,尤其是精胺,以剂量依赖的方式大大降低了与膜结合的蛋白激酶C的量(即处于激活形式的量)。观察到的这种效应具有相当的特异性,因为它取决于多胺的化学结构,并且在微摩尔浓度的聚阳离子时就会显现;效力顺序为精胺>亚精胺>腐胺。本文对这种效应进行了表征,并讨论了其可能的生理意义。

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