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Glycoprotein from street rabies virus BD06 induces early and robust immune responses when expressed from a non-replicative adenovirus recombinant

机译:当由非复制性腺病毒重组体表达时,来自狂犬病狂犬病病毒BD06的糖蛋白可诱导早期和强大的免疫反应

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摘要

The rabies virus (RABV) glycoprotein (G) is responsible for inducing neutralizing antibodies against rabies virus. Development of recombinant vaccines using the G genes from attenuated strains rather than street viruses is a regular practice. In contrast to this scenario, we generated three human adenovirus type 5 recombinants using the G genes from the vaccine strains SRV9 and Flury-LEP, and the street RABV strain BD06 (nrAd5-SRV9-G, nrAd5-Flury-LEP-G, and nrAd5-BD06-G). These recombinants were non-replicative, but could grow up to similar to 10(8) TCID50/ml in helper HEK293AD cells. Expression of the G protein was verified by immunostaining, quantitative PCR and cytometry. Animal experiments revealed that immunization with nrAd5-BD06-G can induce a higher seroconversion rate, a higher neutralizing antibody level, and a longer survival time after rabies virus challenge in mice when compared with the other two recombinants. Moreover, the expression of granulocyte-macrophage colony-stimulating factor (GM-CSF) was significantly higher in mice immunized with nrAd5-BD06-G, which might also contribute to the increased protection. These results show that the use of street RABV G for non-replicative systems may be an alternative for developing effective recombinant rabies vaccines.
机译:狂犬病病毒(RABV)糖蛋白(G)负责诱导针对狂犬病病毒的中和抗体。使用减毒株而不是街头病毒的G基因开发重组疫苗是一种常规做法。与这种情况相反,我们使用来自疫苗株SRV9和Flury-LEP和街头RABV株BD06(nrAd5-SRV9-G,nrAd5-Flury-LEP-G和nrAd5-BD06-G)。这些重组体是非复制性的,但在辅助性HEK293AD细胞中可长至10(8)TCID50 / ml。 G蛋白的表达通过免疫染色,定量PCR和细胞计数法进行验证。动物实验表明,与其他两个重组体相比,用nrAd5-BD06-G免疫可在小鼠中诱导更高的血清转化率,更高的中和抗体水平以及狂犬病毒攻击后更长的存活时间。此外,在用nrAd5-BD06-G免疫的小鼠中,粒细胞巨噬细胞集落刺激因子(GM-CSF)的表达明显更高,这也可能有助于增加保护作用。这些结果表明,将街道RABV G用于非复制系统可能是开发有效的重组狂犬病疫苗的替代方法。

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