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转染人朊病毒蛋白的转基因小鼠慢性传播型朊病毒病的二次传播实验。

Second passage experiments of chronic wasting disease in transgenic mice overexpressing human prion protein.

机构信息

Laboratory of Persistent Viral Diseases, Rocky Mountain Laboratories, National Institute of Allergy and Infectious Diseases, National Institutes of Health, 903 South Fourth Street, Hamilton, MT, 59840, USA.

出版信息

Vet Res. 2022 Dec 16;53(1):111. doi: 10.1186/s13567-022-01130-0.

Abstract

Chronic wasting disease (CWD) is a prion disease of cervids including deer, elk, reindeer, and moose. Human consumption of cervids is common, therefore assessing the risk potential of CWD transmission to humans is critical. In a previous study, we tested CWD transmission via intracerebral inoculation into transgenic mice (tg66 and tgRM) that over-expressed human prion protein. Mice screened by traditional prion detection assays were negative. However, in a group of 88 mice screened by the ultrasensitive RT-QuIC assay, we identified 4 tg66 mice that produced inconsistent positive RT-QuIC reactions. These data could be false positive reactions, residual input inoculum or indicative of subclinical infections suggestive of cross species transmission of CWD to humans. Additional experiments were required to understand the nature of the prion seeding activity in this model. In this manuscript, second passage experiments using brains from mice with weak prion seeding activity showed they were not infectious to additional recipient tg66 mice. Clearance experiments showed that input CWD prion seeding activity was eliminated by 180 days in tg66 mice and PrPKO mice, which are unable to replicate prion protein, indicating that the weak positive levels of seeding activity detected at later time points was not likely residual inoculum. The failure of CWD prions to cause disease in tg66 after two sequential passages suggested that a strong species barrier prevented CWD infection of mice expressing human prion protein.

摘要

慢性消耗病(CWD)是一种影响鹿科动物(包括鹿、麋鹿、驯鹿和驼鹿)的朊病毒病。人类食用鹿科动物的情况很常见,因此评估 CWD 传播给人类的潜在风险至关重要。在之前的一项研究中,我们通过将朊病毒接种到过度表达人类朊病毒蛋白的转基因小鼠(tg66 和 tgRM)的大脑中,来测试 CWD 的传播。通过传统的朊病毒检测方法筛选的小鼠均呈阴性。然而,在一组通过超灵敏 RT-QuIC 检测方法筛选的 88 只小鼠中,我们发现有 4 只 tg66 小鼠产生了不一致的阳性 RT-QuIC 反应。这些数据可能是假阳性反应、残留的接种物,或者表明存在亚临床感染,提示 CWD 可能跨物种传播给人类。需要进行额外的实验来了解该模型中朊病毒接种活性的性质。在本研究中,使用弱朊病毒接种活性的小鼠的脑组织进行的第二代传递实验表明,它们不会感染额外的接受者 tg66 小鼠。清除实验表明,输入的 CWD 朊病毒接种活性在 tg66 小鼠和无法复制朊病毒蛋白的 PrPKO 小鼠中在 180 天后被清除,这表明在后期检测到的较弱的阳性水平的接种活性不太可能是残留的接种物。CWD 朊病毒在两次连续传递后未能引起 tg66 小鼠发病,这表明一个强大的物种障碍阻止了 CWD 感染表达人类朊病毒蛋白的小鼠。

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