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一种用于分析阿尔茨海默病γ-分泌酶的新型底物。

A novel substrate for analyzing Alzheimer's disease gamma-secretase.

作者信息

Lichtenthaler S F, Multhaup G, Masters C L, Beyreuther K

机构信息

Center for Molecular Biology Heidelberg (ZMBH), University of Heidelberg, Germany.

出版信息

FEBS Lett. 1999 Jun 25;453(3):288-92. doi: 10.1016/s0014-5793(99)00730-9.

Abstract

Proteolytic processing of Alzheimer's disease amyloid precursor protein (APP) by beta-secretase leads to A4CT (C99), which is further cleaved by the as yet unknown protease called gamma-secretase. To study the enzymatic properties of gamma-secretase independently of beta-secretase, A4CT together with an N-terminal signal peptide (SPA4CT) may be expressed in eukaryotic cells. However, in all existing SPA4CT proteins the signal peptide is not correctly cleaved upon membrane insertion. Here, we report the generation of a mutated SPA4CT protein that is correctly cleaved by signal peptidase and, thus, identical to the APP-derived A4CT. This novel SPA4CT protein is processed by gamma-secretase in the same manner as APP-derived A4CT and might be valuable for the generation of transgenic animals showing amyloid pathology.

摘要

β-分泌酶对阿尔茨海默病淀粉样前体蛋白(APP)进行蛋白水解加工会产生A4CT(C99),而A4CT会被一种目前尚不清楚的蛋白酶γ-分泌酶进一步切割。为了独立于β-分泌酶研究γ-分泌酶的酶学特性,A4CT可与一个N端信号肽(SPA4CT)一起在真核细胞中表达。然而,在所有现有的SPA4CT蛋白中,信号肽在插入膜后不能被正确切割。在此,我们报告了一种突变的SPA4CT蛋白的产生,该蛋白能被信号肽酶正确切割,因此与APP衍生的A4CT相同。这种新型的SPA4CT蛋白被γ-分泌酶加工的方式与APP衍生的A4CT相同,可能对生成表现出淀粉样病理的转基因动物有价值。

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