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建立辛诺柏病毒传播模型并对其进行特征分析。

Development and Characterization of a Sin Nombre Virus Transmission Model in .

机构信息

Department of Medical Microbiology and Infectious Diseases, University of Manitoba, Winnipeg, MB R3E 0J9, Canada.

Zoonotic Diseases and Special Pathogens, National Microbiology Laboratory, Public Health Agency of Canada, Winnipeg, MB R3E3R2, Canada.

出版信息

Viruses. 2019 Feb 21;11(2):183. doi: 10.3390/v11020183.

Abstract

In North America, Sin Nombre virus (SNV) is the main cause of hantavirus cardiopulmonary syndrome (HCPS), a severe respiratory disease with a fatality rate of 35⁻40%. SNV is a zoonotic pathogen carried by deer mice (), and few studies have been performed examining its transmission in deer mouse populations. Studying SNV and other hantaviruses can be difficult due to the need to propagate the virus in vivo for subsequent experiments. We show that when compared with standard intramuscular infection, the intraperitoneal infection of deer mice can be as effective in producing SNV stocks with a high viral RNA copy number, and this method of infection provides a more reproducible infection model. Furthermore, the age and sex of the infected deer mice have little effect on viral replication and shedding. We also describe a reliable model of direct experimental SNV transmission. We examined the transmission of SNV between deer mice and found that direct contact between deer mice is the main driver of SNV transmission rather than exposure to contaminated excreta/secreta, which is thought to be the main driver of transmission of the virus to humans. Furthermore, increases in heat shock responses or testosterone levels in SNV-infected deer mice do not increase the replication, shedding, or rate of transmission. Here, we have demonstrated a model for the transmission of SNV between deer mice, the natural rodent reservoir for the virus. The use of this model will have important implications for further examining SNV transmission and in developing strategies for the prevention of SNV infection in deer mouse populations.

摘要

在北美,辛诺柏病毒(Sin Nombre virus,SNV)是汉坦病毒心肺综合征(hantavirus cardiopulmonary syndrome,HCPS)的主要病因,这是一种严重的呼吸道疾病,死亡率为 35⁻40%。SNV 是一种由鹿鼠()携带的人畜共患病原体,很少有研究对其在鹿鼠种群中的传播进行研究。由于需要在体内繁殖病毒以进行后续实验,因此研究 SNV 和其他汉坦病毒可能会很困难。我们表明,与标准肌肉内感染相比,鹿鼠的腹腔内感染在产生高病毒 RNA 拷贝数的 SNV 储备方面同样有效,并且这种感染方法提供了更可重复的感染模型。此外,感染鹿鼠的年龄和性别对病毒复制和脱落的影响很小。我们还描述了一种可靠的 SNV 直接实验传播模型。我们研究了 SNV 在鹿鼠之间的传播,发现鹿鼠之间的直接接触是 SNV 传播的主要驱动因素,而不是接触受污染的排泄物/分泌物,后者被认为是病毒传播给人类的主要驱动因素。此外,感染 SNV 的鹿鼠中热休克反应或睾酮水平的增加不会增加病毒的复制、脱落或传播速度。在这里,我们展示了一种在鹿鼠之间传播 SNV 的模型,鹿鼠是该病毒的天然啮齿动物宿主。这种模型的使用将对进一步研究 SNV 传播以及制定预防鹿鼠种群中 SNV 感染的策略具有重要意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cc48/6409794/6c8132961ab0/viruses-11-00183-g001.jpg

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