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酵母蛋白酶A体外自激活的机制及离子依赖性:对体内分区激活的潜在影响

Mechanism and ion-dependence of in vitro autoactivation of yeast proteinase A: possible implications for compartmentalized activation in vivo.

作者信息

Van Den Hazel H, Wolff A M, Kielland-Brandt M C, Winther J R

机构信息

Department of Yeast Genetics, Carlsberg Laboratory, Copenhagen, Denmark.

出版信息

Biochem J. 1997 Sep 1;326 ( Pt 2)(Pt 2):339-44.

Abstract

Yeast proteinase A is synthesized as a zymogen which transits through the endoplasmic reticulum, the Golgi complex and the endosome to the vacuole. On arrival in the vacuole, activation takes place. It has previously been found that proteinase A can activate autocatalytically; however, the propeptide of proteinase A shows essentially no similarity to other known aspartic proteinase propeptides. To understand why proteinase A activation occurs rapidly in the vacuole but not at all in earlier compartments, we have purified the zymogen and investigated the conditions that trigger autoactivation and the mechanism of autoactivation. Autoactivation was triggered by acidic pH and its rate increased with increasing ionic strength. Kinetic evidence indicates that autoactivation mainly occurs via a bimolecular product-catalysed mechanism in which an active proteinase A molecule activates a zymogen molecule. Both the pH- and ionic-strength-dependence and the predominance of a product-catalysed mechanism are well adapted to the situation in vivo, since slow activation in the absence of active proteinase A helps to prevent activation in prevacuolar compartments, whereas, on delivery to the vacuole, lower pH, higher ionic strength and the presence of already active proteinases ensure rapid activation. Product-catalysed autoactivation may be a general mechanism by which cells ensure autoactivation of intracellular enzymes to be both rapid and compartmentalized.

摘要

酵母蛋白酶A最初以酶原形式合成,其经内质网、高尔基体复合体和内体转运至液泡。到达液泡后,激活过程发生。此前已发现蛋白酶A可进行自催化激活;然而,蛋白酶A的前肽与其他已知的天冬氨酸蛋白酶前肽基本没有相似性。为了解为何蛋白酶A的激活在液泡中迅速发生而在早期区室中根本不发生,我们纯化了该酶原,并研究了触发自激活的条件以及自激活的机制。酸性pH触发自激活,且其速率随离子强度增加而加快。动力学证据表明自激活主要通过双分子产物催化机制发生,即一个活性蛋白酶A分子激活一个酶原分子。pH和离子强度依赖性以及产物催化机制的主导地位都很好地适应了体内情况,因为在没有活性蛋白酶A时的缓慢激活有助于防止在前液泡区室中激活,而在转运至液泡时,较低的pH、较高的离子强度以及已存在的活性蛋白酶可确保快速激活。产物催化的自激活可能是细胞确保细胞内酶的自激活既快速又具有区室化的一种普遍机制。

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