化学
生物化学
肽
蛋白酵素
神经退行性变
蛋白酶
劈理(地质)
淀粉样前体蛋白
酶
脑脊液
污渍
体内
阿尔茨海默病
生物
医学
古生物学
生物技术
疾病
病理
神经科学
断裂(地质)
基因
作者
Jan H. Verheijen,L.G.M. Huisman,Natascha van Lent,Ulf Neumann,Paolo Paganetti,C. Erik Hack,Femke H. Bouwman,J. Lindeman,Edward Bollen,Roeland Hanemaaijer
出处
期刊:Clinical Chemistry
[American Association for Clinical Chemistry]
日期:2006-04-14
卷期号:52 (6): 1168-1174
被引量:67
标识
DOI:10.1373/clinchem.2006.066720
摘要
Formation of deposits of the insoluble amyloid beta-peptide is believed to be causally related with neurodegeneration in Alzheimer disease (AD). The beta-peptide originates from a larger amyloid precursor protein (APP) by the action of proteolytic enzymes. The first proteolytic event leading to amyloid formation is the cleavage of APP by the membrane-bound aspartyl protease BACE-1, also known as memapsin-2. Inhibition of BACE-1 is thought to be a therapeutic approach to AD. Measuring BACE-1 activity in biological samples would be useful to elucidate the mechanism of AD and for development of AD drugs.We developed a sensitive and specific activity assay for BACE-1. The assay is based on a genetically engineered proenzyme that is specifically activated by BACE-1. The resulting active enzyme is measured with a chromogenic substrate. The use of 2 coupled reactions produces a detection limit as low as 0.4 pmol/L.The assay detected BACE-1 activity in extracts of human brain tissue as well as, unexpectedly, in human cerebrospinal fluid (CSF). Gel electrophoresis and Western blotting identified the BACE-1 present in CSF as a truncated soluble form of the originally membrane-bound BACE-1.Detection of the soluble form of BACE-1 in CSF, a relatively easily accessible biological fluid, may be useful for monitoring the effects of drug candidates in vivo and may have diagnostic or prognostic applications.
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