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Dissociation between Transmissible Spongiform Encephalopathy (TSE) Infectivity and Proteinase K-Resistant PrPSc Levels in Peripheral Tissue from a Murine Transgenic Model of TSE Disease

机译:小鼠转基因TsE病模型外周组织中传染性海绵状脑病(TsE)感染与蛋白酶K抗性prpsc水平的分离

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摘要

Most current diagnostic tests for transmissible spongiform encephalopathies (TSE) rely on the presence of PK-resistant PrP(Sc) (PrP-res) in post-mortem tissues as indicative of TSE disease. However, a number of studies have highlighted a discrepancy between TSE infectivity and PrP-res levels in both natural and experimental cases of TSE disease. Previously we have shown high TSE infectivity levels in the brain tissue of mice that have a clinical TSE disease with associated vacuolar pathology but little or no PrP-res detectable. Here the levels of TSE infectivity and PrP-res within a peripheral tissue of this mouse model were investigated. Biochemical analysis identified low levels of PrP-res were present in the spleen tissue in comparison to levels observed in the spleen of mice infected with ME7 or 79A. However, upon sub-passage of brain and spleen tissue from clinically ill mice with little or no PrP-res detectable, similar short incubation periods to disease were observed, indicating that infectivity levels were similarly high in both tissues. Thus the discrepancy between PrP-res and TSE infectivity was also present in the peripheral tissues of this disease model. This result indicates that peripheral tissues can contain higher levels of infectivity given the correct combination of host species, PrP genotype and TSE agent. Therefore the assumption that levels of peripheral infectivity are lower than those in the central nervous system is not always correct and could have implications for current food safety regulations.
机译:当前对可传播的海绵状脑病(TSE)的大多数诊断测试都依赖于死后组织中存在PK耐药的PrP(Sc)(PrP-res)作为TSE疾病的征兆。但是,许多研究都强调了自然和实验性TSE疾病中TSE感染性和PrP-res水平之间的差异。以前,我们已经显示了患有临床TSE疾病并伴有液泡病理但很少或没有可检测到的PrP-res的小鼠脑组织中高TSE感染性水平。在这里,研究了该小鼠模型的外周组织中TSE感染性和PrP-res的水平。生化分析表明,与在ME7或79A感染小鼠的脾脏中观察到的水平相比,在脾脏组织中存在低水平的PrP-res。然而,从临床病小鼠的大脑和脾脏组织传代后,几乎没有检测到PrP-res或没有检测到PrP-res,观察到与疾病相似的短潜伏期,这表明两种组织的感染性水平同样较高。因此,在该疾病模型的外周组织中也存在PrP-res和TSE感染性之间的差异。该结果表明,如果宿主物种,PrP基因型和TSE试剂正确组合,外围组织可以包含更高水平的感染力。因此,周围感染水平低于中枢神经系统水平的假设并不总是正确的,并且可能对当前的食品安全法规产生影响。

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    Dobie, Karen; Barron, Rona;

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  • 年度 2013
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  • 正文语种 eng
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