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膜蛋白分泌酶

Membrane protein secretases.

作者信息

Hooper N M, Karran E H, Turner A J

机构信息

Department of Biochemistry and Molecular Biology, University of Leeds, U.K.

出版信息

Biochem J. 1997 Jan 15;321 ( Pt 2)(Pt 2):265-79. doi: 10.1042/bj3210265.

Abstract

A diverse range of membrane proteins of Type 1 or Type II topology also occur as a circulating, soluble form. These soluble forms are often derived from the membrane form by proteolysis by a group of enzymes referred to collectively as 'secretases' or 'sheddases'. The cleavage generally occurs close to the extracellular face of the membrane, releasing physiologically active protein. This secretion process also provides a mechanism for down-regulating the protein at the cell surface. Examples of such post-translational proteolysis are seen in the Alzheimer's amyloid precursor protein, the vasoregulatory enzyme angiotensin converting enzyme, transforming growth factor-alpha, the tumour necrosis factor ligand and receptor superfamilies, certain cytokine receptors, and others. Since the proteins concerned are involved in pathophysiological processes such as neurodegeneration, apoptosis, oncogenesis and inflammation, the secretases could provide novel therapeutic targets. Recent characterization of these individual secretases has revealed common features, particularly sensitivity to certain metalloprotease inhibitors and upregulation of activity by phorbol esters. It is therefore likely that a closely related family of metallosecretases controls the surface expression of multiple integral membrane proteins. Current knowledge of the various secretases are compared in this Review, and strategies for cell-free assays of such proteases are outlined as a prelude to their ultimate purification and cloning.

摘要

具有I型或II型拓扑结构的多种膜蛋白也以循环的可溶性形式存在。这些可溶性形式通常是由一组统称为“分泌酶”或“脱落酶”的酶通过蛋白水解作用从膜形式衍生而来。切割通常发生在靠近膜细胞外表面的位置,释放出生理活性蛋白。这种分泌过程还提供了一种在细胞表面下调该蛋白的机制。这种翻译后蛋白水解的例子可见于阿尔茨海默病淀粉样前体蛋白、血管调节酶血管紧张素转换酶、转化生长因子-α、肿瘤坏死因子配体和受体超家族、某些细胞因子受体等。由于相关蛋白质参与神经退行性变、细胞凋亡、肿瘤发生和炎症等病理生理过程,分泌酶可能提供新的治疗靶点。最近对这些单个分泌酶的表征揭示了共同特征,特别是对某些金属蛋白酶抑制剂的敏感性以及佛波酯对活性的上调作用。因此,很可能是一个密切相关的金属分泌酶家族控制着多种整合膜蛋白的表面表达。本综述比较了目前对各种分泌酶的了解,并概述了此类蛋白酶的无细胞测定策略,作为其最终纯化和克隆的前奏。

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