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通过双重标记免疫组织化学对自然感染羊瘙痒病的绵羊淋巴组织和神经组织中积累朊病毒蛋白(PrPsc)的细胞进行表型分析。

Phenotyping of protein-prion (PrPsc)-accumulating cells in lymphoid and neural tissues of naturally scrapie-affected sheep by double-labeling immunohistochemistry.

作者信息

Andréoletti Olivier, Berthon Patricia, Levavasseur Etienne, Marc Daniel, Lantier Frédéric, Monks Eoin, Elsen Jean-Michel, Schelcher François

机构信息

UMR INRA-ENVT, Physiopathologie Infectieuse et Parasitaire des Ruminants, Ecole Nationale Vétérinaire, Toulouse, France.

出版信息

J Histochem Cytochem. 2002 Oct;50(10):1357-70. doi: 10.1177/002215540205001009.

DOI:10.1177/002215540205001009
PMID:12364569
Abstract

Transmissible spongiform encephalopathies are fatal neurodegenerative diseases characterized by amyloid deposition of protein-prion (PrPsc), the pathogenic isoform of the host cellular protein PrPc, in the immune and central nervous systems. In the absence of definitive data on the nature of the infectious agent, PrPsc immunohistochemistry (IHC) constitutes one of the main methodologies for pathogenesis studies of these diseases. In situ PrPsc immunolabeling requires formalin fixation and paraffin embedding of tissues, followed by post-embedding antigen retrieval steps such as formic acid and hydrated autoclaving treatments. These procedures result in poor cellular antigen preservation, precluding the phenotyping of cells involved in scrapie pathogenesis. Until now, PrPsc-positive cell phenotyping relied mainly on morphological criteria. To identify these cells under the PrPsc IHC conditions, a new, rapid, and highly sensitive PrPsc double-labeling technique was developed, using a panel of screened antibodies that allow specific labeling of most of the cell subsets and structures using paraffin-embedded lymphoid and neural tissues from sheep, leading to an accurate identification of ovine PrPsc-accumulating cells. This technique constitutes a useful tool for IHC investigation of scrapie pathogenesis and may be applicable to the study of other ovine infectious diseases.

摘要

传染性海绵状脑病是致命的神经退行性疾病,其特征是在免疫和中枢神经系统中存在蛋白质朊病毒(PrPsc)的淀粉样沉积,PrPsc是宿主细胞蛋白PrPc的致病异构体。在缺乏关于感染因子性质的确切数据的情况下,PrPsc免疫组织化学(IHC)是这些疾病发病机制研究的主要方法之一。原位PrPsc免疫标记需要对组织进行福尔马林固定和石蜡包埋,然后进行诸如甲酸和水合高压灭菌处理等包埋后抗原修复步骤。这些程序导致细胞抗原保存不佳,排除了对参与羊瘙痒病发病机制的细胞进行表型分析的可能性。到目前为止,PrPsc阳性细胞表型分析主要依赖形态学标准。为了在PrPsc IHC条件下识别这些细胞,开发了一种新的、快速且高度灵敏的PrPsc双重标记技术,使用一组经过筛选的抗体,这些抗体能够使用来自绵羊的石蜡包埋淋巴组织和神经组织对大多数细胞亚群和结构进行特异性标记,从而准确识别绵羊中积累PrPsc的细胞。该技术是用于羊瘙痒病发病机制免疫组织化学研究的有用工具,可能适用于其他绵羊传染病的研究。

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