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牛海绵状脑病和羊瘙痒病对人类潜在传播性的分子评估。

Molecular assessment of the potential transmissibilities of BSE and scrapie to humans.

作者信息

Raymond G J, Hope J, Kocisko D A, Priola S A, Raymond L D, Bossers A, Ironside J, Will R G, Chen S G, Petersen R B, Gambetti P, Rubenstein R, Smits M A, Lansbury P T, Caughey B

机构信息

Rocky Mountain Laboratories, NIAID, National Institutes of Health, Hamilton, Montana 59840, USA.

出版信息

Nature. 1997 Jul 17;388(6639):285-8. doi: 10.1038/40876.

Abstract

More than a million cattle infected with bovine spongiform encephalopathy (BSE) may have entered the human food chain. Fears that BSE might transmit to man were raised when atypical cases of Creutzfeldt-Jakob disease (CJD), a human transmissible spongiform encephalopathy (TSE), emerged in the UK. In BSE and other TSE diseases, the conversion of the protease-sensitive host prion protein (PrP-sen) to a protease-resistant isoform (PrP-res) is an important event in pathogenesis. Biological aspects of TSE diseases are reflected in the specificities of in vitro PrP conversion reactions. Here we show that there is a correlation between in vitro conversion efficiencies and known transmissibilities of BSE, sheep scrapie and CJD. On this basis, we used an in vitro system to gauge the potential transmissibility of scrapie and BSE to humans. We found limited conversion of human PrP-sen to PrP-res driven by PrP-res associated with both scrapie (PrP[Sc]) and BSE (PrP[BSE]). The efficiencies of these heterologous conversion reactions were similar but much lower than those of relevant homologous conversions. Thus the inherent ability of these infectious agents of BSE and scrapie to affect humans following equivalent exposure may be finite but similarly low.

摘要

超过100万头感染了牛海绵状脑病(BSE)的牛可能已进入人类食物链。当英国出现克雅氏病(CJD)的非典型病例(一种人类可传播的海绵状脑病(TSE))时,人们开始担心BSE可能会传染给人类。在BSE和其他TSE疾病中,蛋白酶敏感的宿主朊病毒蛋白(PrP-sen)转化为蛋白酶抗性异构体(PrP-res)是发病机制中的一个重要事件。TSE疾病的生物学特性反映在体外PrP转化反应的特异性上。在此我们表明,体外转化效率与BSE、羊瘙痒病和CJD的已知传播性之间存在相关性。在此基础上,我们使用体外系统来评估瘙痒病和BSE对人类的潜在传播性。我们发现,与羊瘙痒病(PrP[Sc])和BSE(PrP[BSE])相关的PrP-res驱动人类PrP-sen向PrP-res的转化有限。这些异源转化反应的效率相似,但远低于相关同源转化的效率。因此,在同等暴露后,这些BSE和瘙痒病传染源影响人类的内在能力可能有限,但同样较低。

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