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Yellow Fever Virus/Dengue-2 Virus and Yellow Fever Virus/Dengue-4 Virus Chimeras: Biological Characterization, Immunogenicity, and Protection against Dengue Encephalitis in the Mouse Model

机译:黄热病病毒/登革热2病毒和黄热病病毒/登革热4病毒嵌合体:小鼠模型中的生物学特征,免疫原性和对登革热脑炎的防护

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摘要

Two yellow fever virus (YFV)/dengue virus chimeras which encode the prM and E proteins of either dengue virus serotype 2 (dengue-2 virus) or dengue-4 virus within the genome of the YFV 17D strain (YF5.2iv infectious clone) were constructed and characterized for their properties in cell culture and as experimental vaccines in mice. The prM and E proteins appeared to be properly processed and glycosylated, and in plaque reduction neutralization tests and other assays of antigenic specificity, the E proteins exhibited profiles which resembled those of the homologous dengue virus serotypes. Both chimeric viruses replicated in cell lines of vertebrate and mosquito origin to levels comparable to those of homologous dengue viruses but less efficiently than the YF5.2iv parent. YFV/dengue-4 virus, but not YFV/dengue-2 virus, was neurovirulent for 3-week-old mice by intracerebral inoculation; however, both viruses were attenuated when administered by the intraperitoneal route in mice of that age. Single-dose inoculation of either chimeric virus at a dose of 105 PFU by the intraperitoneal route induced detectable levels of neutralizing antibodies against the homologous dengue virus strains. Mice which had been immunized in this manner were fully protected from challenge with homologous neurovirulent dengue viruses by intracerebral inoculation compared to unimmunized mice. Protection was associated with significant increases in geometric mean titers of neutralizing antibody compared to those for unimmunized mice. These data indicate that YFV/dengue virus chimeras elicit antibodies which represent protective memory responses in the mouse model of dengue encephalitis. The levels of neurovirulence and immunogenicity of the chimeric viruses in mice correlate with the degree of adaptation of the dengue virus strain to mice. This study supports ongoing investigations concerning the use of this technology for development of a live attenuated viral vaccine against dengue viruses.
机译:两种黄热病病毒(YFV)/登革热病毒嵌合体,它们编码YFV 17D菌株(YF5.2iv感染性克隆)基因组中的登革热病毒血清型2(登革热2病毒)或登革热4病毒的prM和E蛋白。构建并表征了它们在细胞培养中的特性以及在小鼠中作为实验疫苗的特性。 prM和E蛋白似乎经过适当加工和糖基化,在噬菌斑减少中和测试和其他抗原特异性测定中,E蛋白表现出与同源登革病毒血清型相似的特征。两种嵌合病毒均在脊椎动物和蚊子起源的细胞系中复制,其水平可与同源登革病毒相媲美,但效率不及YF5.2iv亲本。通过脑内接种,YFV /登革热4病毒对3周龄小鼠具有神经毒性,但对YFV /登革热2病毒无毒。然而,当通过该年龄小鼠的腹膜内途径施用时,两种病毒均减毒。通过腹膜内途径以105 PFU的剂量对两种嵌合病毒进行单剂量接种,可检测到可检测水平的针对同源登革热病毒株的中和抗体。与未免疫的小鼠相比,通过脑内接种完全保护了以这种方式免疫的小鼠免受同源神经毒力登革热病毒的攻击。与未免疫小鼠相比,保护作用与中和抗体几何平均滴度的显着提高有关。这些数据表明YFV /登革热病毒嵌合体在登革热脑炎的小鼠模型中引起代表保护性记忆反应的抗体。嵌合病毒在小鼠中的神经毒性和免疫原性水平与登革热病毒株对小鼠的适应程度有关。这项研究支持正在进行的有关使用该技术开发抗登革热减毒活疫苗的研究。

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