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PNAS Plus: Cofactor molecules maintain infectious conformation and restrict strain properties in purified prions

机译:PNAS Plus:辅因子分子可保持感染性构象并限制纯化purified病毒中的菌株特性

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摘要

Prions containing misfolded prion protein (PrPSc) can be formed with cofactor molecules using the technique of serial protein misfolding cyclic amplification. However, it remains unknown whether cofactors materially participate in maintaining prion conformation and infectious properties. Here we show that withdrawal of cofactor molecules during serial propagation of purified recombinant prions caused adaptation of PrPSc structure accompanied by a reduction in specific infectivity of >105-fold, to undetectable levels, despite the ability of adapted “protein-only” PrPSc molecules to self-propagate in vitro. We also report that changing only the cofactor component of a minimal reaction substrate mixture during serial propagation induced major changes in the strain properties of an infectious recombinant prion. Moreover, propagation with only one functional cofactor (phosphatidylethanolamine) induced the conversion of three distinct strains into a single strain with unique infectious properties and PrPSc structure. Taken together, these results indicate that cofactor molecules can regulate the defining features of mammalian prions: PrPSc conformation, infectivity, and strain properties. These findings suggest that cofactor molecules likely are integral components of infectious prions.
机译:使用序列蛋白错折叠循环扩增技术,可以与辅因子分子形成包含错误折叠的病毒蛋白(PrP Sc )的病毒。然而,尚不知道辅因子是否实质性参与维持maintaining病毒构象和传染性。在这里,我们表明,在纯化的重组病毒的系列繁殖过程中,辅因子分子的撤回导致PrP Sc 结构的适应性降低,同时特异性感染力降低了> 10 5 倍,尽管具有适应性的“仅蛋白质” PrP Sc 分子能够在体外自我传播,但仍无法检测到水平。我们还报告说,在连续传播过程中仅改变最小反应底物混合物的辅因子成分,会引起感染性重组病毒的应变特性发生重大变化。此外,仅用一种功能性辅助因子(磷脂酰乙醇胺)进行繁殖,即可将三种不同的菌株转化为具有独特感染特性和PrP Sc 结构的单一菌株。综上所述,这些结果表明辅因子分子可以调节哺乳动物病毒的定义特征:PrP Sc 构象,感染性和菌株特性。这些发现表明辅因子分子可能是感染性病毒的组成部分。

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