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Prion protein polymorphisms associated with reduced CWD susceptibility limit peripheral PrP CWD deposition in orally infected white-tailed deer

机译:与降低CWD敏感性相关的Prion蛋白多态性限制了口腔感染白尾鹿的外周PrP CWD沉积

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Chronic wasting disease (CWD) is a prion disease affecting members of the Cervidae family. PrPC primary structures play a key role in CWD susceptibility resulting in extended incubation periods and regulating the propagation of CWD strains. We analyzed the distribution of abnormal prion protein (PrPCWD) aggregates in brain and peripheral organs from orally inoculated white-tailed deer expressing four different PRNP genotypes: Q95G96/Q95G96 (wt/wt), S96/wt, H95/wt and H95/S96 to determine if there are substantial differences in the deposition pattern of PrPCWD between different PRNP genotypes. Although we detected differences in certain brain areas, globally, the different genotypes showed similar PrPCWD deposition patterns in the brain. However, we found that clinically affected deer expressing H95 PrPC, despite having the longest survival periods, presented less PrPCWD immunoreactivity in particular peripheral organs. In addition, no PrPCWD was detected in skeletal muscle of any of the deer. Our data suggest that expression of H95-PrPC limits peripheral accumulation of PrPCWD as detected by immunohistochemistry. Conversely, infected S96/wt and wt/wt deer presented with similar PrPCWD peripheral distribution at terminal stage of disease, suggesting that the S96-PrPC allele, although delaying CWD progression, does not completely limit the peripheral accumulation of the infectious agent.
机译:慢性消耗性疾病(CWD)是一种affecting病毒疾病,会影响Cervidae家族的成员。 PrPC的一级结构在CWD敏感性中起关键作用,从而延长了潜伏期并调节了CWD菌株的繁殖。我们分析了表达四种不同PRNP基因型的经口接种的白尾鹿脑和外围器官中蛋白异常蛋白(PrPCWD)聚集体的分布:Q95G96 / Q95G96(wt / wt),S96 / wt,H95 / wt和H95 / S96确定在不同的PRNP基因型之间PrPCWD的沉积模式是否存在实质性差异。尽管我们检测到某些大脑区域存在差异,但总体而言,不同的基因型在大脑中显示出相似的PrPCWD沉积模式。但是,我们发现,尽管具有最长的生存期,但表达H95 PrPC的受临床影响的鹿在特定的外周器官中呈现出较少的PrPCWD免疫反应性。此外,在任何一只鹿的骨骼肌中均未检测到PrPCWD。我们的数据表明,H95-PrPC的表达限制了免疫组织化学检测到的PrPCWD的外周积累。相反,受感染的S96 / wt和wt / wt鹿在疾病末期表现出相似的PrPCWD周边分布,这表明S96-PrPC等位基因虽然延迟了CWD的进程,但并未完全限制感染因子的周边积累。

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