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小鼠神经球的朊病毒感染

Prion infection of mouse neurospheres.

作者信息

Giri Ranjit K, Young Rebecca, Pitstick Rose, DeArmond Stephen J, Prusiner Stanley B, Carlson George A

机构信息

McLaughlin Research Institute, Great Falls, MT 59405, USA.

出版信息

Proc Natl Acad Sci U S A. 2006 Mar 7;103(10):3875-80. doi: 10.1073/pnas.0510902103. Epub 2006 Feb 22.

Abstract

Only a few cell lines have been infected with prions, offering limited genetic diversity and sensitivity to several strains. Here we report that cultured neurospheres expressing cellular prion protein (PrP(C)) can be infected with prions. Neurosphere lines isolated from the brains of mice at embryonic day 13-15 grow as aggregates and contain CNS stem cells. We produced neurosphere cultures from FVB/NCr (FVB) mice, from transgenic (Tg) FVB mice that overexpress mouse PrP-A (Tg4053), and from congenic FVB mice with a targeted null mutation in the PrP gene (Prnp(0/0)) and incubated them with the Rocky Mountain Laboratory prion strain. While monitoring the levels of disease-causing PrP (PrP(Sc)) at each passage, we observed a dramatic rise in PrP(Sc) levels with time in the Tg4053 neurosphere cells, whereas the level of PrP(Sc) decayed to undetectable levels in cell cultures lacking PrP. PrP(Sc) levels in cultures from FVB mice initially declined but then increased with passage. Prions produced in culture were transmissible to mice and produced disease pathology. Intracellular aggregates of PrP(Sc) were present in cells from infected cultures. The susceptibility of neurosphere cultures to prions mirrored that of the mice from which they were derived. Neurosphere lines from Tg4053 mice provide a sensitive in vitro bioassay for mouse prions; neurosphere lines from other Tg mice overexpressing PrP might be used to assay prions from other species, including humans.

摘要

仅有少数细胞系感染过朊病毒,其遗传多样性有限,对几种毒株的敏感性也较低。在此我们报告,表达细胞朊蛋白(PrP(C))的培养神经球可被朊病毒感染。从胚胎第13 - 15天小鼠大脑分离得到的神经球系以聚集体形式生长,并含有中枢神经系统干细胞。我们用来自FVB/NCr(FVB)小鼠、过表达小鼠PrP - A的转基因(Tg)FVB小鼠(Tg4053)以及PrP基因发生靶向无效突变的同基因FVB小鼠(Prnp(0/0))建立了神经球培养物,并使其与落基山实验室朊病毒株孵育。在监测每一代致病型PrP(PrP(Sc))水平时,我们观察到Tg4053神经球细胞中PrP(Sc)水平随时间急剧上升,而在缺乏PrP的细胞培养物中,PrP(Sc)水平衰减至无法检测到的水平。FVB小鼠培养物中的PrP(Sc)水平最初下降,但随后随传代增加。培养物中产生的朊病毒可传播给小鼠并引发疾病病理变化。感染培养物的细胞中存在PrP(Sc)的细胞内聚集体。神经球培养物对朊病毒的易感性与其来源小鼠的易感性一致。Tg4053小鼠的神经球系为小鼠朊病毒提供了一种灵敏的体外生物测定方法;来自其他过表达PrP的Tg小鼠的神经球系可能用于检测包括人类在内的其他物种的朊病毒。

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