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反刍动物朊病毒在绵羊转基因小鼠模型中表现出明显的脾嗜性。

Prions of ruminants show distinct splenotropisms in an ovine transgenic mouse model.

机构信息

Agence Française de Sécurité Sanitaire des Aliments - Lyon, Unité ATNC, Lyon, France.

出版信息

PLoS One. 2010 Apr 26;5(4):e10310. doi: 10.1371/journal.pone.0010310.

Abstract

BACKGROUND

Transmissible agents involved in prion diseases differ in their capacities to target different regions of the central nervous system and lymphoid tissues, which are also host-dependent.

METHODOLOGY/PRINCIPAL FINDINGS: Protease-resistant prion protein (PrP(res)) was analysed by Western blot in the spleen of transgenic mice (TgOvPrP4) that express the ovine prion protein under the control of the neuron-specific enolase promoter, after infection by intra-cerebral route with a variety of transmissible spongiform encephalopathies (TSEs) from cattle and small ruminants. Splenic PrP(res) was consistently detected in classical BSE and in most natural scrapie sources, the electrophoretic pattern showing similar features to that of cerebral PrP(res). However splenic PrP(res) was not detected in L-type BSE and TME-in-cattle, or in the CH1641 experimental scrapie isolate, indicating that some TSE strains showed reduced splenotropism in the ovine transgenic mice. In contrast with CH1641, PrP(res) was also consistently detected in the spleen of mice infected with six natural "CH1641-like" scrapie isolates, but then showed clearly different molecular features from those identified in the brains (unglycosylated PrP(res) at approximately 18 kDa with removal of the 12B2 epitope) of ovine transgenic mice or of sheep. These features included different cleavage of the main PrP(res) cleavage product (unglycosylated PrP(res) at approximately 19 kDa with preservation of the 12B2 epitope) and absence of the additional C-terminally cleaved PrP(res) product (unglycosylated form at approximately 14 kDa) that was detected in the brain.

CONCLUSION/SIGNIFICANCE: Studies in a transgenic mouse model expressing the sheep prion protein revealed different capacities of ruminant prions to propagate in the spleen. They showed unexpected features in "CH1641-like" ovine scrapie suggesting that such isolates contain mixed conformers with distinct capacities to propagate in the brain or lymphoid tissues of these mice.

摘要

背景

与朊病毒病相关的可传播病原体在靶向中枢神经系统和淋巴组织的不同区域方面存在差异,而这些差异也依赖于宿主。

方法/主要发现:在感染了来自牛和小反刍动物的各种传染性海绵状脑病(TSEs)后,通过脑内途径,用转基因组(TgOvPrP4)的绵羊朊病毒蛋白在脾中进行了蛋白酶抗性朊病毒蛋白(PrP(res))的 Western blot 分析。在经典 BSE 和大多数天然瘙痒病来源中,脾 PrP(res) 一直被检测到,其电泳图谱与脑 PrP(res) 的特征相似。然而,L 型 BSE 和 TME 在牛中,或在 CH1641 实验性瘙痒病分离株中,未检测到脾 PrP(res),这表明一些 TSE 株在绵羊转基因小鼠中显示出较低的脾嗜性。与 CH1641 相反,脾 PrP(res) 也一直被感染六种天然“CH1641 样”瘙痒病分离株的小鼠所检测到,但随后与在绵羊转基因小鼠或绵羊脑中鉴定的分子特征明显不同(未糖基化的 PrP(res) 约 18 kDa,失去 12B2 表位)。这些特征包括主要 PrP(res) 切割产物的不同切割(未糖基化的 PrP(res) 约 19 kDa,保留 12B2 表位)和不存在在脑中检测到的额外 C 端切割的 PrP(res)产物(未糖基化形式约 14 kDa)。

结论/意义:在表达绵羊朊病毒蛋白的转基因小鼠模型中进行的研究表明,反刍动物朊病毒在脾脏中具有不同的繁殖能力。它们在“CH1641 样”绵羊瘙痒病中表现出出乎意料的特征,表明这些分离株含有具有不同能力在这些小鼠的大脑或淋巴组织中繁殖的混合构象。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/311d/2859945/50482f8a418d/pone.0010310.g001.jpg

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