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扩展人类降解组的复杂性:多聚酶及其串联丝氨酸蛋白酶结构域

Expanding the complexity of the human degradome: polyserases and their tandem serine protease domains.

作者信息

Cal Santiago, Moncada-Pazos Angela, Lopez-Otin Carlos

机构信息

Departamento de Bioquimica y Biologia Molecular, Facultad de Medicina, Instituto Universitario de Oncologia, Universidad de Oviedo, Oviedo, Asturias, Spain.

出版信息

Front Biosci. 2007 May 1;12:4661-9. doi: 10.2741/2415.

Abstract

The large and growing number of protease genes identified in the human genome, more than 560, reflects the complexity and relevance of these enzymes in multiple biological processes. As part of our studies on the human degradome--which is defined as the complete set of human protease genes--we have recently identified and cloned three complex polyserine proteases called polyserases. Polyserase-1 is a member of the type-II transmembrane serine protease (TTSP) family of proteolytic enzymes that undergoes a series of post-translational processing events to generate three distinct and independent serine protease domains called serase-1, -2, and -3. Polyserase-2 is a secreted enzyme that also possesses three serine protease domains, but they remain as an integral part of the initial protein product. Finally, polyserase-3 is also a secreted enzyme that contains two serine protease domains embedded in the same polypeptide chain. Despite all three human polyserases share this complex molecular design characterized by the presence of several catalytic domains in their structure, they also exhibit distinctive features including unique expression patterns and different enzymatic properties. At present, the putative functional advantages derived from the complex structural organization of polyserases remain unknown, but the widespread occurrence of these enzymes in mammalian degradomes provides additional evidence about the complexity of proteolytic systems in these organisms.

摘要

在人类基因组中已鉴定出大量且数量不断增加的蛋白酶基因,超过560个,这反映了这些酶在多种生物过程中的复杂性和相关性。作为我们对人类降解组(定义为人类蛋白酶基因的完整集合)研究的一部分,我们最近鉴定并克隆了三种复杂的多丝氨酸蛋白酶,称为多聚酶。多聚酶-1是II型跨膜丝氨酸蛋白酶(TTSP)家族的蛋白水解酶成员,它经历一系列翻译后加工事件,产生三个不同且独立的丝氨酸蛋白酶结构域,称为丝氨酸酶-1、-2和-3。多聚酶-2是一种分泌型酶,也拥有三个丝氨酸蛋白酶结构域,但它们仍然是初始蛋白质产物的一个组成部分。最后,多聚酶-3也是一种分泌型酶,其在同一多肽链中包含两个丝氨酸蛋白酶结构域。尽管所有三种人类多聚酶都具有这种复杂的分子设计,其结构中存在几个催化结构域,但它们也表现出独特的特征,包括独特的表达模式和不同的酶学性质。目前,多聚酶复杂结构组织所带来的假定功能优势仍然未知,但这些酶在哺乳动物降解组中的广泛存在为这些生物体中蛋白水解系统的复杂性提供了额外证据。

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