Division of Virology, Department of Microbiology and Immunology, Institute of Medical Science, University of Tokyo, Tokyo, Japan.
J Virol. 2013 Jul;87(14):7874-81. doi: 10.1128/JVI.00076-13. Epub 2013 May 8.
Vaccination is an effective means to protect against influenza virus. Although inactivated and live-attenuated vaccines are currently available, each vaccine has disadvantages (e.g., immunogenicity and safety issues). To overcome these problems, we previously developed a replication-incompetent PB2-knockout (PB2-KO) influenza virus that replicates only in PB2 protein-expressing cells. Here, we generated two PB2-KO viruses whose PB2-coding regions were replaced with the HA genes of either A/California/04/2009 (H1N1pdm09) or A/Vietnam/1203/2004 (H5N1). The resultant viruses comparably, or in some cases more efficiently, induced virus-specific antibodies in the serum, nasal wash, and bronchoalveolar lavage fluid of mice relative to a conventional formalin-inactivated vaccine. Furthermore, mice immunized with these PB2-KO viruses were protected from lethal challenges with not only the backbone virus strain but also strains from which their foreign HAs originated, indicating that PB2-KO viruses with antigenically different HAs could serve as bivalent influenza vaccines.
接种疫苗是预防流感病毒的有效手段。目前已有灭活疫苗和减毒活疫苗,但每种疫苗都有其缺点(例如免疫原性和安全性问题)。为了克服这些问题,我们之前开发了一种复制缺陷型 PB2 敲除(PB2-KO)流感病毒,该病毒仅在表达 PB2 蛋白的细胞中复制。在这里,我们生成了两种 PB2-KO 病毒,其 PB2 编码区被替换为 A/加利福尼亚/04/2009(H1N1pdm09)或 A/越南/1203/2004(H5N1)的 HA 基因。与传统的甲醛灭活疫苗相比,这些病毒在血清、鼻腔冲洗液和支气管肺泡灌洗液中诱导病毒特异性抗体的能力相当,在某些情况下甚至更高。此外,用这些 PB2-KO 病毒免疫的小鼠不仅能抵抗骨架病毒株的致死性挑战,还能抵抗其外来 HA 来源的株的致死性挑战,表明具有不同抗原性的 PB2-KO 病毒可以作为二价流感疫苗。
