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首页> 外文期刊>Theranostics >Visualization of a neurotropic flavivirus infection in mouse reveals unique viscerotropism controlled by host type I interferon signaling
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Visualization of a neurotropic flavivirus infection in mouse reveals unique viscerotropism controlled by host type I interferon signaling

机译:小鼠中嗜神经性黄病毒感染的可视化揭示了受宿主I型干扰素信号传导控制的独特内脏

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摘要

Flavivirus includes a large group of human pathogens with medical importance. Especially, neurotropic flaviviruses capable of invading central and peripheral nervous system, e.g. Japanese encephalitis virus (JEV) and Zika virus (ZIKV), are highly pathogenic to human and constitute major global health problems. However, the dynamic dissemination and pathogenesis of neurotropic flavivirus infections remain largely unknown. Here, using JEV as a model, we rationally designed and constructed a recombinant reporter virus that stably expressed Renilla luciferase (Rluc). The resulting JEV reporter virus (named Rluc-JEV) and parental JEV exhibited similar replication and infection characteristics, and the magnitude of Rluc activity correlated well with progeny viral production in vitro and in vivo . By using in vivo bioluminescence imaging (BLI) technology, we dissected the replication and dissemination dynamics of JEV infection in mice upon different inoculation routes. Interestingly, besides replicating in mouse brain, Rluc-JEV predominantly invaded the abdominal organs in mice with typical viscerotropism. Further tests in mice deficient in type I interferon (IFN) receptors demonstrated robust and prolonged viral replication in the intestine, spleen, liver, kidney and other abdominal organs. Combined with histopathological and immunohistochemical results, the host type I IFN signaling was evidenced as the major barrier to the viscerotropism and pathogenicity of this neurotropic flavivirus. Additionally, the Rluc-JEV platform was readily adapted for efficacy assay of known antiviral compounds and a live JE vaccine. Collectively, our study revealed abdominal organs as important targets of JEV infection in mice and profiled the unique viscerotropism trait controlled by the host type I IFN signaling. This in vivo visualization technology described here provides a powerful tool for testing antiviral agents and vaccine candidates for flaviviral infection.
机译:黄病毒包括一大批具有医学重要性的人类病原体。尤其是,能够侵袭中枢神经系统和周围神经系统的嗜神经性黄病毒。日本脑炎病毒(JEV)和寨卡病毒(ZIKV)对人类具有高致病性,并构成主要的全球健康问题。然而,神经营养性黄病毒感染的动态传播和发病机理仍然未知。在这里,我们以JEV为模型,合理设计并构建了稳定表达海肾荧光素酶(Rluc)的重组报告病毒。产生的JEV报告病毒(命名为Rluc-JEV)和亲本JEV表现出相似的复制和感染特性,并且Rluc活性的大小与体内外子代病毒的产生密切相关。通过使用体内生物发光成像(BLI)技术,我们剖析了不同接种途径下JEV感染在小鼠中的复制和传播动力学。有趣的是,除了在小鼠大脑中复制外,Rluc-JEV还以典型的内向性侵染小鼠的主要器官。在缺乏I型干扰素(IFN)受体的小鼠中进行的进一步测试表明,病毒在肠道,脾脏,肝脏,肾脏和其他腹部器官中的复制旺盛而持久。结合组织病理学和免疫组化结果,宿主I型IFN信号被证明是这种嗜神经性黄病毒的内向性和致病性的主要障碍。此外,Rluc-JEV平台可轻松用于已知抗病毒化合物和活性JE疫苗的功效分析。总的来说,我们的研究揭示了腹腔器官是小鼠JEV感染的重要目标,并概述了由宿主I型IFN信号传导控制的独特的内向性性状。此处描述的这种体内可视化技术为测试抗病毒剂和候选疫苗的黄病毒感染提供了强大的工具。

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