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A recombinant rabies virus expressing vesicular stomatitis virus glycoprotein fails to protect against rabies virus infection

机译:表达水疱性口炎病毒的重组狂犬病毒 糖蛋白不能预防狂犬病毒感染

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摘要

To investigate the importance of the rabies virus (RV) glycoprotein (G) in protection against rabies, we constructed a recombinant RV (rRV) in which the RV G ecto- and transmembrane domains were replaced with the corresponding regions of vesicular stomatitis virus (VSV) glycoprotein (rRV-VSV-G). We were able to recover rRV-VSV-G and found that particle production was equal to rRV. However, the budding of the chimeric virus was delayed and infectious titers were reduced 10-fold compared with the parental rRV strain containing RV G. Biochemical analysis showed equal replication rates of both viruses, and similar amounts of wild-type and chimeric G were present in the respective viral particles. Additional studies were performed to determine whether the immune response against rRV-VSV-G was sufficient to protect against rabies. Mice were primed with rRV or rRV-VSV-G and challenged with a pathogenic strain of RV 12 days later. Similar immune responses against the internal viral proteins of both viruses indicated successful infection. All mice receiving the rRV vaccine survived the challenge, whereas immunization with rRV-VSV-G did not induce protection. The results confirm the crucial role of RV G in an RV vaccine.
机译:为了研究狂犬病病毒(RV)糖蛋白(G)在预防狂犬病中的重要性,我们构建了重组RV(rRV),其中RV G的外膜和跨膜结构域被水疱性口炎病毒(VSV)的相应区域代替)糖蛋白(rRV-VSV-G)。我们能够回收rRV-VSV-G,发现颗粒产量与rRV相等。但是,与含有RV G的亲本rRV株相比,嵌合病毒的出芽被延迟了,并且感染的滴度降低了10倍。生化分析表明两种病毒的复制率相同,并且存在相似量的野生型和嵌合G在各自的病毒颗粒中。进行了其他研究,以确定针对rRV-VSV-G的免疫反应是否足以预防狂犬病。用rRV或rRV-VSV-G引发小鼠,并在12天后用RV的致病株攻击。针对两种病毒内部病毒蛋白的相似免疫反应表明感染成功。接受rRV疫苗的所有小鼠均在攻击中存活,而使用rRV-VSV-G的免疫未诱导 保护。结果证实了RV G在RV中的关键作用 疫苗。

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