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首页> 外文期刊>Virology >Comparative studies of infectivity, immunogenicity and cross-protective efficacy of live attenuated influenza vaccines containing nucleoprotein from cold-adapted or wild-type influenza virus in a mouse model
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Comparative studies of infectivity, immunogenicity and cross-protective efficacy of live attenuated influenza vaccines containing nucleoprotein from cold-adapted or wild-type influenza virus in a mouse model

机译:在小鼠模型中,含有核蛋白的活衰减流感疫苗的感染性,免疫原性和交叉保护功效的比较研究

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摘要

This study sought to improve an existing live attenuated influenza vaccine (LAW) by including nucleoprotein (NP) from wild-type virus rather than master donor virus (MDV). H7N9 LAIV reassortants with 6:2 (NP from MDV) and 5:3 (NP from wild-type virus) genome compositions were compared with regard to their growth characteristics, induction of humoral and cellular immune responses in mice, and ability to protect mice against homologous and heterologous challenge viruses. Although, in general, the 6:2 reassortant induced greater cell mediated immunity in C57BL6 mice than the 5:3 vaccine, mice immunized with the 5:3 LAIV were better protected against heterologous challenge. The 5:3 LAIV-induced CTLs also had better in vivo killing activity against target cells loaded with the NP366 epitope of recent influenza viruses. Modification of the genome of reassortant vaccine viruses by incorporating the NP gene from wild-type viruses represents a simple strategy to improve the immunogenicity and cross-protection of influenza vaccines.
机译:该研究寻求通过包括来自野生型病毒的核蛋白(NP)来改善现有的活病变型流感疫苗(法律),而不是母型病毒(MDV)。与6:2(来自MDV的NP)和5:3(来自野生型病毒的NP)的H7N9 LaV重新归断与小鼠的生长特性,诱导小鼠的体液和细胞免疫应答以及保护小鼠的能力进行比较基因组组合物针对同源和异源攻击病毒。虽然通常,6:2重新分化诱导的C57BL6小鼠中的更高细胞介导的免疫比5:3疫苗,用5:3 Laiv免疫的小鼠进行免受异源攻击的影响。 5:3 Laiv诱导的CTL还更好地体内杀伤活性,针对近期流感病毒的NP366表位负载的靶细胞。通过将NP基因从野生型病毒结合到改善流感疫苗的免疫原性和交叉保护来改变重配疫苗病毒的改性。

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