Hope J, Morton L J, Farquhar C F, Multhaup G, Beyreuther K, Kimberlin R H
EMBO J. 1986 Oct;5(10):2591-7. doi: 10.1002/j.1460-2075.1986.tb04539.x.
Scrapie-associated fibrils (SAF) are unique structures characteristic of the group of unconventional slow infections which includes scrapie and Creutzfeldt-Jakob disease. A major component of hamster fibrils has been described as a protease-resistant glycoprotein with an apparent mol. wt of 27,000-30,000 (PrP27-30). However, we report here that if fibrils are prepared by procedures designed to minimise proteolysis the PrP proteins co-purifying with hamster SAF have mol. wts of 33,000-35,000 (PrP33-35) and 26,000-29,000 (PrP26-29). We find a Lys-Lys-Arg-Pro-Lys sequence at the amino terminus of these SAF proteins, that is absent from PrP27-30, and which has recently been predicted to be the N-terminal sequence of the native PrP protein of uninfected brain. The major SAF protein (PrP33-35) and its normal brain homologue are shown to have the same apparent mol. wt and ionic charge distribution by two-dimensional gel analysis, silver staining and immunoblotting. These results support our view that PrP33-35 and the normal brain PrP protein may have the same covalent structure, and that the PrP protein is recruited into these amyloid-like SAF or into association with a non-protein component of SAF by an irreversible event initiated directly or indirectly by scrapie infection.
瘙痒病相关纤维(SAF)是一组非常规慢感染所特有的独特结构,这组感染包括瘙痒病和克雅氏病。仓鼠纤维的主要成分被描述为一种分子量约为27,000 - 30,000的抗蛋白酶糖蛋白(PrP27 - 30)。然而,我们在此报告,如果通过旨在最小化蛋白水解的程序制备纤维,与仓鼠SAF共纯化的PrP蛋白分子量为33,000 - 35,000(PrP33 - 35)和26,000 - 29,000(PrP26 - 29)。我们在这些SAF蛋白的氨基末端发现了一个Lys - Lys - Arg - Pro - Lys序列,该序列在PrP27 - 30中不存在,并且最近被预测为未感染大脑中天然PrP蛋白的N末端序列。通过二维凝胶分析、银染和免疫印迹显示,主要的SAF蛋白(PrP33 - 35)及其正常脑同源物具有相同的表观分子量和离子电荷分布。这些结果支持我们的观点,即PrP33 - 35和正常脑PrP蛋白可能具有相同的共价结构,并且PrP蛋白通过瘙痒病感染直接或间接引发的不可逆事件被招募到这些淀粉样SAF中或与SAF的非蛋白质成分结合。
