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新型人呼吸道合胞病毒小鼠模型中的长期感染与发病机制

Long-Term Infection and Pathogenesis in a Novel Mouse Model of Human Respiratory Syncytial Virus.

机构信息

National Rodent Laboratory Animal Resources Center, Institute for Laboratory Animal Resources, National Institutes for Food and Drug Control (NIFDC), Beijing 102629, China.

Department of Microbiology & Infectious Disease Center, School of Basic Medical Sciences, Peking University Health Science Center, Beijing 100083, China.

出版信息

Viruses. 2022 Aug 9;14(8):1740. doi: 10.3390/v14081740.

Abstract

Intensive efforts have been made to develop models of hRSV infection or disease using various animals. However, the limitations such as semi-permissiveness and short duration of infection have impeded their applications in both the pathogenesis of hRSV and therapeutics development. Here, we present a mouse model based on a gene knockout using CRISPR/Cas9 technology. Rag2 mice sustained high viral loads upon intranasal inoculation with hRSV. The average peak titer rapidly reached 1 × 10 copies/g and 1c10 TCID in nasal cavity, as well as 1 × 10 copies/g and 1 × 10 TCID in the lungs up to 5 weeks. Mild interstitial pneumonia, severe bronchopneumonia, elevated cytokines and NK cells were seen in Rag2 mice. A humanized monoclonal antibody showed strong antiviral activity in this animal model, implying that Rag2 mice that support long-term stable infection are a useful tool for studying the transmission and pathogenesis of human RSV, as well as evaluating therapeutics.

摘要

已经做出了巨大努力,利用各种动物来开发 hRSV 感染或疾病模型。然而,这些模型存在半许可性和感染持续时间短等局限性,限制了它们在 hRSV 发病机制和治疗药物开发中的应用。在这里,我们使用 CRISPR/Cas9 技术展示了一种基于基因敲除的小鼠模型。Rag2 小鼠在鼻腔接种 hRSV 后可维持高病毒载量。鼻腔中的平均峰值滴度迅速达到 1×10 拷贝/g 和 1c10 TCID,肺部中的病毒滴度也分别达到 1×10 拷贝/g 和 1×10 TCID,持续长达 5 周。Rag2 小鼠中可见轻度间质性肺炎、严重细支气管炎、细胞因子和 NK 细胞升高。在这种动物模型中,一种人源化单克隆抗体显示出很强的抗病毒活性,这表明支持长期稳定感染的 Rag2 小鼠是研究人呼吸道合胞病毒传播和发病机制以及评估治疗药物的有用工具。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c455/9415064/7f7cac3e4317/viruses-14-01740-g001.jpg

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