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关于小鼠、绵羊和牛朊病毒蛋白中物种特异性表位的研究。

Studies on a species-specific epitope in murine, ovine and bovine prion protein.

作者信息

Groschup M H, Pfaff E

机构信息

Federal Research Centre for Virus Diseases of Animals, Tübingen, Germany.

出版信息

J Gen Virol. 1993 Jul;74 ( Pt 7):1451-6. doi: 10.1099/0022-1317-74-7-1451.

Abstract

Transmissible spongiform encephalopathies are fatal neurodegenerative disorders which are linked to abnormal isoforms of the prion protein (PrP), which is expressed in different cells of various mammalian species. Susceptibility to disease and reduced transmission rates upon the first passage to another species are thought to be a result of functional and biochemical differences of the PrP as a consequence of amino acid sequence among species. In 1985 an epidemic of bovine spongiform encephalopathy (BSE) started after accidental transmission of scrapie by feeding infected sheep and goat meat and bone meal products to cattle. In this report we present data demonstrating species-specific epitopes in bovine, ovine and murine PrP that are based on amino acid substitutions at positions 108 and 110. Rabbit antisera to synthetic peptides representing amino acid sequence 108 to 123 of PrP of cattle, sheep and mice reacted strongly with modified PrP of the homologous host but not, or only poorly, with PrP of heterogeneous origin. Cross-reactivity was observed, however, with antisera to bovine and ovine peptide sequences 102 to 117, thus stressing the importance of the location of the amino acid substitution in synthetic peptides used for immunization. Based on these data, BSE PrP and ovine and murine scrapie PrP can be distinguished from each other, and these differences might help elucidate the species barrier effect.

摘要

传染性海绵状脑病是致命的神经退行性疾病,与朊病毒蛋白(PrP)的异常异构体有关,该蛋白在各种哺乳动物物种的不同细胞中表达。疾病易感性以及首次传播到另一个物种时传播率降低被认为是由于物种间氨基酸序列导致PrP功能和生化差异的结果。1985年,牛海绵状脑病(BSE)疫情在将感染羊瘙痒病的羊和山羊肉骨粉产品喂给牛后意外传播后开始。在本报告中,我们展示了基于牛、羊和鼠PrP中第108和110位氨基酸取代的物种特异性表位的数据。针对代表牛、羊和小鼠PrP氨基酸序列108至123的合成肽的兔抗血清与同源宿主的修饰PrP强烈反应,但与异源PrP反应微弱或不反应。然而,观察到针对牛和羊肽序列102至117的抗血清存在交叉反应,从而强调了用于免疫的合成肽中氨基酸取代位置的重要性。基于这些数据,BSE PrP与羊和鼠瘙痒病PrP可以相互区分,这些差异可能有助于阐明物种屏障效应。

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