首页> 美国卫生研究院文献>Journal of Virology >Proteinase K-Resistant Material in ARR/VRQ Sheep Brain Affected with Classical Scrapie Is Composed Mainly of VRQ Prion Protein
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Proteinase K-Resistant Material in ARR/VRQ Sheep Brain Affected with Classical Scrapie Is Composed Mainly of VRQ Prion Protein

机译:VRQ on蛋白主要由ARR / VRQ绵羊脑中耐蛋白酶K的材料组成受经典刮伤的影响。

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摘要

Classical scrapie is a prion disease in sheep and goats. In sheep, susceptibility to disease is genetically influenced by single amino acid substitutions. Genetic breeding programs aimed at enrichment of arginine-171 (171R) prion protein (PrP), the so-called ARR allele, in the sheep population have been demonstrated to be effective in reducing the occurrence of classical scrapie in the field. Understanding the molecular basis for this reduced prevalence would serve the assessment of ARR adaptation. The prion formation mechanism and conversion of PrP from the normal form (PrPC) to the scrapie-associated form (PrPSc) could play a key role in this process. Therefore, we investigated whether the ARR allele substantially contributes to scrapie prion formation in naturally infected heterozygous 171Q/R animals. Two methods were applied to brain tissue of 171Q/R heterozygous sheep with natural scrapie to determine the relative amount of the 171R PrP fraction in PrPres, the proteinase K-resistant PrPSc core. An antibody test differentiating between 171Q and 171R PrP fragments showed that PrPres was mostly composed of the 171Q allelotype. Furthermore, using a novel tool for prion research, endoproteinase Lys-C-digested PrPres yielded substantial amounts of a nonglycosylated and a monoglycosylated PrP fragment comprising codons 114 to 188. Following two-dimensional gel electrophoresis, only marginal amounts (<9%) of 171R PrPres were detected. Enhanced 171Rres proteolytic susceptibility could be excluded. Thus, these data support a nearly zero contribution of 171R PrP in PrPres of 171R/Q field scrapie-infected animals. This is suggestive of a poor adaptation of classical scrapie to this resistance allele under these natural conditions.
机译:古典瘙痒病是绵羊和山羊的a病毒病。在绵羊中,疾病易感性在遗传上受单个氨基酸取代的影响。事实证明,旨在提高绵羊种群中精氨酸171(171R)ion病毒蛋白(PrP)(即所谓的ARR等位基因)的遗传育种程序可有效减少野外经典瘙痒病的发生。了解这种减少患病率的分子基础将有助于评估ARR适应性。 ion病毒的形成机理以及PrP从正常形式(PrP C )转变为瘙痒病相关形式(PrP Sc )的过程可能起关键作用。因此,我们调查了ARR等位基因是否在自然感染的杂合171Q / R动物中实质上促进了瘙痒病pr病毒的形成。两种方法分别用天然瘙痒病对171Q / R杂合绵羊的脑组织进行测定,以确定PrP res (耐K蛋白酶的PrP Sc 核心。区分171Q和171R PrP片段的抗体测试表明,PrP res 主要由171Q等位基因组成。此外,使用一种新型的病毒研究工具,内蛋白酶Lys-C消化的PrP res 产生了大量的非糖基化和单糖基化的PrP片段,其密码子为114至188。在二维凝胶电泳后,仅检测到171R PrP res 的边缘量(<9%)。可以排除增强的171R res 蛋白水解敏感性。因此,这些数据支持171R PrP在171R / Q田间被痒病感染的动物的PrP res 中的贡献几乎为零。这表明在这些自然条件下经典瘙痒病很难适应该抗性等位基因。

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