首页> 外文期刊>Viral immunology >Protective Immunity Against Homologous and Heterologous Influenza Virus Lethal Challenge by Immunization with New Recombinant Chimeric HA2-M2e Fusion Protein in BALB/C Mice
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Protective Immunity Against Homologous and Heterologous Influenza Virus Lethal Challenge by Immunization with New Recombinant Chimeric HA2-M2e Fusion Protein in BALB/C Mice

机译:通过在BALB / C小鼠中使用新的重组嵌合HA2-M2e融合蛋白免疫来抵抗同源和异源流感病毒致死性攻击的保护性免疫

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摘要

Influenza is an acute and highly contagious respiratory disease. The error prone RNA polymerase and segmented nature of the influenza A virus genome allow antigenic drift and shift, respectively. Therefore, most influenza vaccines are inefficient along time and against different viral subtypes. In this study, for the first time, protection properties of a new recombinant fusion of HA2 and M2e peptides originated from influenza virus A/Brisbane/59/2007-like (H1N1) in BALB/c mice model were investigated. After immunization of the BALB/c mice, the protection property of fusion peptide was determined by a neutralizing assay test. For further study, mice were lethal challenged by the (mouse adapted, A/PR8/34 [H1N1]) and heterologous (mouse adapted, A/Brisbane/10/2007 [H3N2]) influenza virus subtypes. Then, the lung viral titers, body weight, and survival rate of the immunized mice were monitored. The results showed that immunization by the M2e-HA2 recombinant fusion peptide provides strong protection against homologous challenge and an infirm protection against heterologous. These protections against homologous and heterologous influenza A virus challenges meant the universal nature of these recombinant peptides in an immunity manner against influenza A virus. However, more studies are needed to optimize this recombinant construction, and this experiment recommends HA2-M2e fusion peptide as a universal influenza A vaccine candidate.
机译:流感是一种急性和高度传染性的呼吸系统疾病。容易出错的RNA聚合酶和甲型流感病毒基因组的片段性质分别使抗原漂移和移位。因此,大多数流感疫苗随着时间的推移以及针对不同病毒亚型的效率均不高。在这项研究中,首次研究了一种新的流感病毒A / Brisbane / 59 / 2007-like(H1N1)来源的HA2和M2e肽重组融合体在BALB / c小鼠模型中的保护特性。免疫BALB / c小鼠后,通过中和试验测试确定融合肽的保护特性。为了进一步研究,小鼠被(小鼠适应的,A / PR8 / 34 [H1N1])和异源(小鼠适应的,A / Brisbane / 10/2007 [H3N2])流感病毒致死性攻击。然后,监测免疫小鼠的肺病毒滴度,体重和存活率。结果表明,通过M2e-HA2重组融合肽进行的免疫提供了针对同源攻击的强力保护和针对异源的弱保护。这些针对同源和异源甲型流感病毒的保护措施意味着这些重组肽具有针对甲型流感病毒的免疫力,具有普遍性。但是,需要更多的研究来优化这种重组构建,并且该实验建议将HA2-M2e融合肽用作通用的A型流感疫苗候选者。

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