首页> 美国卫生研究院文献>The Journal of General Virology >Stability of murine scrapie strain 87V after passage in sheep and comparison with the CH1641 ovine strain
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Stability of murine scrapie strain 87V after passage in sheep and comparison with the CH1641 ovine strain

机译:鼠羊瘙痒病毒株在绵羊传代后的稳定性及与CH1641绵羊毒株的比较

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摘要

Breed- and prion protein (PRNP) genotype-related disease phenotype variability has been observed in sheep infected with the 87V murine scrapie strain. Therefore, the stability of this strain was tested by inoculating sheep-derived 87V brain material back into VM mice. As some sheep-adapted 87V disease phenotypes were reminiscent of CH1641 scrapie, transgenic mice (Tg338) expressing ovine prion protein (PrP) were inoculated with the same sheep-derived 87V sources and with CH1641. Although at first passage in VM mice the sheep-derived 87V sources showed some divergence from the murine 87V control, all the characteristics of murine 87V infection were recovered at second passage from all sheep sources. These included 100 % attack rates and indistinguishable survival times, lesion profiles, immunohistochemical features of disease-associated PrP accumulation in the brain and PrP biochemical properties. All sheep-derived 87V sources, as well as CH1641, were transmitted to Tg338 mice with identical clinical, pathological, immunohistochemical and biochemical features. While this might potentially indicate that sheep-adapted 87V and CH1641 are the same strain, profound divergences were evident, as murine 87V was unable to infect Tg338 mice but was lethal for VM mice, while the reverse was true for CH1641. These combined data suggest that: (i) murine 87V is stable and retains its properties after passage in sheep; (ii) it can be isolated from sheep showing a CH1641-like or a more conventional scrapie phenotype; and (iii) sheep-adapted 87V scrapie, with conventional or CH1641-like phenotype, is biologically distinct from experimental CH1641 scrapie, despite the fact that they behave identically in a single transgenic mouse line.  
机译:在感染了87V鼠痒病菌株的绵羊中已观察到与病毒和病毒蛋白(PRNP)基因型相关的疾病表型变异。因此,通过将绵羊来源的87V脑材料接种回VM小鼠中来测试该菌株的稳定性。由于一些适应绵羊的87V疾病表型让人联想到CH1641瘙痒病,因此,用相同的绵羊来源的87V来源和CH1641接种了表达绵羊病毒蛋白(PrP)的转基因小鼠(Tg338)。尽管在VM小鼠的第一个传代中,绵羊来源的87V来源与鼠87V对照显示出一些差异,但第二次传代时从所有绵羊来源恢复了鼠87V感染的所有特征。其中包括100%的发作率和难以区分的生存时间,病变情况,与疾病相关的PrP在脑中积累的免疫组织化学特征和PrP的生化特性。所有绵羊来源的87V来源以及CH1641均被传播到具有相同临床,病理,免疫组织化学和生化特征的Tg338小鼠。尽管这可能表明适应绵羊的87V和CH1641是同一株,但明显的分歧是显而易见的,因为鼠87V无法感染Tg338小鼠,但对VM小鼠具有致命性,而CH1641则相反。这些综合数据表明:(i)鼠87V是稳定的,并且在传给绵羊后仍保持其特性; (ii)可以从显示出CH1641样或更常规的瘙痒病表型的绵羊中分离得到; (iii)具有常规或CH1641样表型的绵羊适应性87V瘙痒病,在生物学上不同于实验性CH1641瘙痒病,尽管它们在单个转基因小鼠品系中表现相同。

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