首页> 美国卫生研究院文献>Journal of Virology >Chimeric Yellow Fever/Dengue Virus as a Candidate Dengue Vaccine: Quantitation of the Dengue Virus-Specific CD8 T-Cell Response
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Chimeric Yellow Fever/Dengue Virus as a Candidate Dengue Vaccine: Quantitation of the Dengue Virus-Specific CD8 T-Cell Response

机译:嵌合黄热病/登革热病毒作为候选登革热疫苗:登革热病毒特异性CD8 T细胞反应的定量

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摘要

We have constructed a chimeric yellow fever/dengue (YF/DEN) virus, which expresses the premembrane (prM) and envelope (E) genes from DEN type 2 (DEN-2) virus in a YF virus (YFV-17D) genetic background. Immunization of BALB/c mice with this chimeric virus induced a CD8 T-cell response specific for the DEN-2 virus prM and E proteins. This response protected YF/DEN virus-immunized mice against lethal dengue encephalitis. Control mice immunized with the parental YFV-17D were not protected against DEN-2 virus challenge, indicating that protection was mediated by the DEN-2 virus prM- and E-specific immune responses. YF/DEN vaccine-primed CD8 T cells expanded and were efficiently recruited into the central nervous systems of DEN-2 virus challenged mice. At 5 days after challenge, 3 to 4% of CD8 T cells in the spleen were specific for the prM and E proteins, and 34% of CD8 T cells in the central nervous system recognized these proteins. Depletion of either CD4 or CD8 T cells, or both, strongly reduced the protective efficacy of the YF/DEN virus, stressing the key role of the antiviral T-cell response.
机译:我们构建了一种嵌合黄热病/登革热(YF / DEN)病毒,该病毒在YF病毒(YFV-17D)的遗传背景下表达DEN 2型(DEN-2)病毒的前膜(prM)和包膜(E)基因。用这种嵌合病毒对BALB / c小鼠进行免疫诱导了对DEN-2病毒prM和E蛋白具有特异性的CD8 T细胞应答。这种反应可以保护YF / DEN病毒免疫小鼠免于致命的登革热脑炎。用亲本YFV-17D免疫的对照小鼠没有受到DEN-2病毒攻击的保护,表明该保护作用是由DEN-2病毒prM和E特异性免疫反应介导的。 YF / DEN疫苗引发的CD8 T细胞扩增,并有效地募集到DEN-2病毒攻击小鼠的中枢神经系统中。攻击后第5天,脾脏中3-4%的CD8 T细胞对prM和E蛋白具有特异性,中枢神经系统中34%的CD8 T细胞识别这些蛋白。 CD4或CD8 T细胞或两者的耗尽会大大降低YF / DEN病毒的保护功效,从而强调抗病毒T细胞反应的关键作用。

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