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用流感和腺病毒对 Toxoplasma gondii 表面抗原 2(SAG2)进行初免和加强免疫可诱导强烈的保护性免疫。

Prime and boost immunization with influenza and adenovirus encoding the Toxoplasma gondii surface antigen 2 (SAG2) induces strong protective immunity.

机构信息

Departamento de Bioquímica e Imunologia, Instituto de Ciências Biológicas, Universidade Federal de Minas Gerais, Belo Horizonte 31270-910, MG, Brazil.

出版信息

Vaccine. 2010 Apr 19;28(18):3247-56. doi: 10.1016/j.vaccine.2010.02.003. Epub 2010 Feb 26.

Abstract

In this work, we explored an original vaccination protocol using recombinant influenza and adenovirus. We constructed recombinant influenza viruses harboring dicistronic NA segments containing the surface antigen 2 (SAG2) from Toxoplasma gondii under control of the duplicated 3' promoter. Recombinant influenza viruses were able to drive the expression of the foreign SAG2 sequence in cell culture and to replicate efficiently both in cell culture and in lungs of infected mice. In addition, mice primed with recombinant influenza virus and boosted with a recombinant adenovirus encoding SAG2 elicited both humoral and cellular immune responses specific for SAG2. Moreover, when immunized animals were challenged with the cystogenic P-Br strain of T. gondii, they displayed up to 85% of reduction in parasite burden. These results demonstrate the potential use of recombinant influenza vectors harboring the dicistronic segments in the development of vaccines against infectious diseases.

摘要

在这项工作中,我们探索了一种使用重组流感病毒和腺病毒的原始疫苗接种方案。我们构建了携带含有弓形虫表面抗原 2(SAG2)双顺反子 NA 片段的重组流感病毒,该片段受重复 3'启动子的控制。重组流感病毒能够在细胞培养物中驱动外源 SAG2 序列的表达,并在细胞培养物和感染小鼠的肺部中高效复制。此外,用编码 SAG2 的重组腺病毒对用重组流感病毒进行初次免疫和加强免疫的小鼠引发了针对 SAG2 的体液和细胞免疫反应。此外,当免疫动物受到弓形虫的囊生 P-Br 株的挑战时,它们的寄生虫负荷减少了高达 85%。这些结果表明,携带双顺反子片段的重组流感载体在开发针对传染病的疫苗方面具有潜在用途。

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