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Molecular mass biochemical composition and physicochemical behavior of the infectious form of the scrapie precursor protein monomer.

机译:瘙痒病前体蛋白单体传染形式的分子量生化组成和理化行为。

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摘要

A highly purified fraction obtained from scrapie (263-K strain)-infected hamsters' brains by an alternative procedure without proteinase K treatment contained a protease-resistant form of the scrapie precursor protein (PrPSc) and infectivity of 9.9 +/- 0.7 log LD50/ml. Polyclonal antibodies produced against hamster scrapie amyloid protein (PrP27-30) and used in a neutralization test diminished infectivity of the PrPSc preparations by 1.6 log after intracerebral inoculation and by 1 log after intraperitoneal inoculation. PrPSc was subjected to size-exclusion HPLC; greater than or equal to 60% of the eluted infectious units were recovered from the peak with an apparent mass of 30.4 +/- 0.6 kDa. Characterization by UV absorption spectra, SDS/PAGE, immunoblots, N-terminal amino acid sequence, and neutral sugar and amino sugar analyses demonstrated homogeneity of the infectious units. The neutral sugar and amino sugar compositional analyses revealed high mannose, glucosamine, fucose, and sialic acid content. This demonstrated an extensive posttranslational modification by the complex type of N-linked glycosylation and glycane core of C-terminal glycolipid of PrPSc. The results correspond to the predicted size, composition, and sequence of PrPSc and indicate that this protein may be the only component of scrapie infectious unit or the infectious form of scrapie precursor.
机译:通过不经蛋白酶K处理的另一种方法,从被瘙痒病(263-K株)感染的仓鼠的大脑中获得的高纯度级分,含有蛋白酶抵抗性的瘙痒病前体蛋白(PrPSc),传染性为9.9 +/- 0.7 log LD50 /毫升。产生针对仓鼠瘙痒性淀粉样蛋白(PrP27-30)的多克隆抗体,并用于中和测试,可将PrPSc制剂的感染性在脑内接种后降低1.6 log,在腹膜内接种后降低1 log。 PrPSc进行体积排阻HPLC;从峰中回收了大于或等于60%的洗脱感染单位,表观质量为30.4 +/- 0.6 kDa。通过紫外吸收光谱,SDS / PAGE,免疫印迹,N末端氨基酸序列以及中性糖和氨基糖分析进行表征,证明了感染单位的均质性。中性糖和氨基糖成分分析表明,甘露糖,葡糖胺,岩藻糖和唾液酸含量较高。这表明N-连接的糖基化和PrPSc的C端糖脂的甘氨酸核心的复杂类型对翻译进行了广泛的修饰。结果与PrPSc的预测大小,组成和序列相对应,表明该蛋白可能是瘙痒病感染单位的唯一成分或瘙痒病前体的感染形式。

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