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Disease phenotype in sheep after infection with cloned murine scrapie strains

机译:克隆的鼠瘙痒病菌感染后绵羊的疾病表型

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摘要

Prion diseases exhibit different disease phenotypes in their natural hosts and when transmitted to rodents, and this variability is regarded as indicative of prion strain diversity. Phenotypic characterization of scrapie strains in sheep can be attempted by histological, immunohistochemical and biochemical approaches, but it is widely considered that strain confirmation and characterization requires rodent bioassay. Examples of scrapie strains obtained from original sheep isolates by serial passage in mice include ME7, 79A, 22A and 87V. In order to address aspects of prion strain stability across the species barrier, we transmitted the above murine strains to sheep of different breeds and susceptible Prnp genotypes. The experiment included 40 sheep dosed by the oral route alone and 36 sheep challenged by combined subcutaneous and intracerebral routes. Overall, the combined route produced higher attack rates (~100%) than the oral route (~50%) and 2-4 times shorter incubation periods. Uniquely, 87V given orally was unable to infect any sheep. Overall, scrapie strains adapted and cloned in mice produce distinct but variable disease phenotypes in sheep depending on breed or Prnp genotype. Further re-isolation experiments in mice are in progress in order to determine whether the original cloned murine disease phenotype will reemerge.
机译:on病毒在其天然宿主中和传播给啮齿动物时表现出不同的疾病表型,这种变异被认为是病毒菌株多样性的指示。绵羊瘙痒病菌株的表型鉴定可以通过组织学,免疫组织化学和生化方法进行尝试,但人们普遍认为,菌株的确认和鉴定需要啮齿动物的生物测定。通过在小鼠中连续传代而从原始绵羊分离物中获得的瘙痒病菌株的实例包括ME7、79A,22A和87V。为了解决跨物种障碍的病毒菌株稳定性的各个方面,我们将上述鼠种菌株传播给了不同品种和易感Prnp基因型的绵羊。该实验包括40只通过口服途径给药的绵羊和36只通过皮下和脑内结合途径挑战的绵羊。总体而言,联合途径的侵袭率(〜100%)高于口服途径(〜50%),潜伏期缩短了2-4倍。独特的是,口服给予的87V电压无法感染任何绵羊。总体而言,适应和克隆在小鼠中的瘙痒病菌株在绵羊中会产生不同但可变的疾病表型,具体取决于品种或Prnp基因型。为了确定原始克隆的鼠类疾病表型是否会重新出现,正在小鼠中进行进一步的分离实验。

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