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首页> 外文期刊>Journal of Virological Methods >Strategies to obtain multiple recombinant modified vaccinia Ankara vectors. Applications to influenza vaccines
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Strategies to obtain multiple recombinant modified vaccinia Ankara vectors. Applications to influenza vaccines

机译:获得多重重组改性痘苗病毒载体的策略。 应用于流感疫苗

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摘要

As a vaccination vector, MVA has been widely investigated both in animal models and humans. The construction of recombinant MVA (rMVA) relies on homologous recombination between an acceptor virus and a donor plasmid in infected/transfected permissive cells. Our construction strategy "Red-to-Green gene swapping" - based on the exchange of two fluorescent markers within the flanking regions of MVA deletion Delta III, coupled to fluorescence activated cell sorting - is here extended to a second insertion site, within the flanking regions of MVA deletion Delta VI. Exploiting this strategy, both double and triple rMVA were constructed, expressing as transgenes the influenza A proteins HA, NP, M1, and PB1. Upon validation of the harbored transgenes co-expression, double and triple recombinants rMVA(Delta III)-NP-P2A-M1 and rMVA(Delta III)-NP-P2A-M1-(Delta VI)-PB1 were assayed for in vivo immunogenicity and protection against lethal challenge. In vivo responses were identical to those obtained with the reported combinations of single recombinants, supporting the feasibility and reliability of the present improvement and the extension of Red-to-Green gene swapping to insertion sites other than Delta III.
机译:作为疫苗接种载体,MVA在动物模型和人类中被广泛研究。重组MVA(RMVA)的构建依赖于受感染/转染允许细胞中受体病毒和供体质粒之间的同源重组。我们的建设策略“红绿色基因交换” - 基于MVA缺失ΔIII的侧翼区域内的两个荧光标记的交换,耦合到荧光活性细胞分选 - 此处延伸到侧翼内的第二插入部位MVA删除Delta VI的区域。利用这种策略,构建双和三重RMVA,表达为转基因的流感蛋白质HA,NP,M1和PB1。在验证哈博尔转基因时,共表达,双重组腺素RMVA(Delta III)-NP-P2A-M1和RMVA(Delta III)-NP-P2A-M1-(Delta VI)-PB1以体内免疫原性测定并防止致命挑战。在体内反应与通过报告的单一重组剂组合获得的反应相同,支持本出改善的可行性和可靠性和延伸红细胞基因交换到Delta III以外的插入位点。

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