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不同的羊瘙痒病朊病毒分离株在转基因小鼠和仓鼠大脑中的复制具有区域特异性。

Replication of distinct scrapie prion isolates is region specific in brains of transgenic mice and hamsters.

作者信息

Hecker R, Taraboulos A, Scott M, Pan K M, Yang S L, Torchia M, Jendroska K, DeArmond S J, Prusiner S B

机构信息

Department of Neurology, University of California, San Francisco 94143.

出版信息

Genes Dev. 1992 Jul;6(7):1213-28. doi: 10.1101/gad.6.7.1213.

Abstract

Scrapie prions are composed largely, if not entirely, of PrPSc molecules. The prion isolates Sc237 and 139H exhibit markedly different incubation times in Syrian, Armenian, and Chinese hamsters, as well as in transgenic (Tg) 81 mice expressing Syrian hamster PrP (SHaPrP). Repassage of prions from transgenic mice or Chinese hamsters into Syrian hamsters revealed that the original properties of the prion isolates are retained. When Syrian hamsters were first inoculated with 139H prions and subsequently challenged with Sc237 prions, the incubation period was determined by the faster Sc237 isolate. Regional mapping studies demonstrated different kinetics and patterns of PrPSc accumulation for Sc237 and 139H prions in the brains of Syrian hamsters as well as Tg(SHaPrP)7 mice. That distinct prion isolates induce different region-specific accumulations of PrPSc in brain suggests a novel mechanism for propagation of isolates whereby they replicate in particular sets of neurons. The prion isolates could be targeted to specific CNS cells by differing conformations of PrPSc, post-translational modifications of PrPSc such as Asn-linked glycosylation, or an as yet undetected macromolecule complexed with PrPSc in the prion.

摘要

痒病朊病毒即使不是完全由PrPSc分子组成,也主要由其组成。朊病毒分离株Sc237和139H在叙利亚仓鼠、亚美尼亚仓鼠和中国仓鼠以及表达叙利亚仓鼠PrP(SHaPrP)的转基因(Tg)81小鼠中表现出明显不同的潜伏期。将朊病毒从转基因小鼠或中国仓鼠传代至叙利亚仓鼠后发现,朊病毒分离株的原始特性得以保留。当叙利亚仓鼠首先接种139H朊病毒,随后再用Sc237朊病毒攻击时,潜伏期由更快的Sc237分离株决定。区域定位研究表明,Sc237和139H朊病毒在叙利亚仓鼠以及Tg(SHaPrP)7小鼠大脑中的PrPSc积累具有不同的动力学和模式。不同的朊病毒分离株在大脑中诱导不同区域特异性的PrPSc积累,这提示了一种新的分离株传播机制,即它们在特定的神经元组中复制。朊病毒分离株可能通过PrPSc的不同构象、PrPSc的翻译后修饰(如N-连接糖基化)或与朊病毒中PrPSc复合的尚未检测到的大分子靶向特定的中枢神经系统细胞。

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