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使用生物发光报告病毒对小鼠黄热病病毒感染进行可视化观察。

Visualization of yellow fever virus infection in mice using a bioluminescent reporter virus.

作者信息

Dong Hao-Long, Wang Hong-Jiang, Liu Zhong-Yu, Ye Qing, Qin Xiao-Ling, Li Dan, Deng Yong-Qiang, Jiang Tao, Li Xiao-Feng, Qin Cheng-Feng

机构信息

State Key Laboratory of Pathogen and Biosecurity, Institute of Microbiology and Epidemiology, Academy of Military Medical Sciences, Beijing, People's Republic of China.

Department of Comprehensive Basic Experiment, The Chinese People's Liberation Army Strategic Support Force Characteristic Medical Center, Beijing, People's Republic of China.

出版信息

Emerg Microbes Infect. 2021 Dec;10(1):1739-1750. doi: 10.1080/22221751.2021.1967705.

Abstract

Yellow fever virus (YFV) is a re-emerging flavivirus, which can lead to severe clinical manifestations and high mortality, with no specific antiviral therapies available. The live-attenuated yellow fever vaccine 17D (YF17D) has been widely used for over eighty years. However, the emergence of yellow fever vaccine-associated viscerotropic disease (YFL-AVD) and yellow fever vaccine-associated neurotropic disease (YFL-AND) raised non-negligible concerns. Additionally, the attenuation mechanism of YF17D is still unclear. Thus, the development of convenient models is crucial to understand the mechanisms behind YF17D attenuation and its adverse effects. In this work, we generated a reporter YF17D expressing nano-luciferase (NLuc). and characterization demonstrated that the NLuc-YF17D shared similar biological properties with its parental strain and the NLuc activity can reflect viral infectivity reliably. Combined with bioluminescence imaging, a series of mice models of YF17D infection was established, which will be useful for the evaluation of antiviral medicines and novel vaccine candidates. Especially, we demonstrated that intraperitoneally (i.p.) infection of NLuc-YF17D in type I interferon receptor-deficient mice A129 resulted in outcomes resembling YEL-AVD and YEL-AND, evidenced by viral replication in multiple organs and invasion of the central neuronal system. Finally, and assays based on this reporter virus were established to evaluate the antiviral activities of validated antiviral agents. In conclusion, the bioluminescent reporter virus described herein provides a powerful platform to study YF17D attenuation and vaccine-associated diseases as well as to develop novel countermeasures against YFV.

摘要

黄热病病毒(YFV)是一种再度出现的黄病毒,可导致严重的临床表现和高死亡率,且目前尚无特异性抗病毒疗法。减毒活疫苗黄热病17D(YF17D)已广泛使用八十多年。然而,黄热病疫苗相关内脏嗜性疾病(YFL-AVD)和黄热病疫苗相关神经嗜性疾病(YFL-AND)的出现引发了不可忽视的担忧。此外,YF17D的减毒机制仍不清楚。因此,开发便捷的模型对于理解YF17D减毒背后的机制及其不良反应至关重要。在这项工作中,我们构建了一种表达纳米荧光素酶(NLuc)的报告基因YF17D。特性表征表明,NLuc-YF17D与其亲本毒株具有相似的生物学特性,且NLuc活性能够可靠地反映病毒感染性。结合生物发光成像技术,建立了一系列YF17D感染小鼠模型,这将有助于评估抗病毒药物和新型候选疫苗。特别是,我们证明在I型干扰素受体缺陷小鼠A129中腹腔内(i.p.)感染NLuc-YF17D会导致类似于黄热病疫苗相关内脏嗜性疾病(YEL-AVD)和黄热病疫苗相关神经嗜性疾病(YEL-AND)的结果,多个器官中的病毒复制以及中枢神经系统的侵袭证明了这一点。最后,基于这种报告病毒建立了检测方法以评估经过验证的抗病毒药物的抗病毒活性。总之,本文所述的生物发光报告病毒为研究YF17D减毒和疫苗相关疾病以及开发针对YFV的新型对策提供了一个强大的平台。

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