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首页> 外文期刊>Vaccine >Evaluation of the protective immunity of the Legionella pneumophila recombinant protein FlaA/MompS/PilE in an A/J mouse model.
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Evaluation of the protective immunity of the Legionella pneumophila recombinant protein FlaA/MompS/PilE in an A/J mouse model.

机译:A / J小鼠模型中的军团乳突肺炎肺炎肺炎的保护性免疫的评价ZHSE / J小鼠模型中的重组蛋白FLAA / MOMPS /桩。

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To investigate the protect effects of the recombinant protein FlaA/MompS/PilE against Legionella pneumophila (L. pneumophila), the coding sequences of the three proteins were optimized by DNA Star software firstly, cloned, expressed by Escherichia coli BL21, and purified. To give an enhanced the immunological response, the proteins were linked together with (Linker) or without a linker insert (NLinker) and were purified from E. coli BL21. The A/J mouse model was used to determine the level of the induction of protective immunity from the purified proteins. Our results showed that the IgG titer, which was measured by ELISA, was increased after the administration of the five proteins. Compared to the administration of the individual proteins, the chimeric Linker and NLinker proteins displayed lasting immunity to a lethal dose of L. pneumophila challenge. The Linker protein protected the A/J mouse against a higher dose of L. pneumonia compared to the other proteins used in this study, as it contained a more effective immunogen. The work presented here demonstrates that the bioinformatics software, DNA Star, is a valid tool to analyse the epitopes of proteins and was useful in the optimization of proteins that could induce the protective immune response to L. pneumophila. The cross-immunity of recombinant proteins, such as the Linker and the NLinker chimera, have higher generates a greater immune than the single proteins.Digital Object Identifier http://dx.doi.org/10.1016/j.vaccine.2011.03.010
机译:为了研究重组蛋白FLAA / MOMPS / MOMPS / MOMPS / MOMPS /堆对军团肺炎( L.PNEumophila BL21。 A / J小鼠模型用于确定来自纯化蛋白质的保护性免疫诱导的水平。我们的研究结果表明,在施用五种蛋白质后,通过ELISA测量的IgG滴度。与单个蛋白质的给药相比,嵌合接头和Nlinker蛋白显示持续免疫的致命剂量的 l。肺炎 - / i>挑战。接头蛋白质保护A / J小鼠均针对较高剂量的 L保护A / J小鼠。肺炎与本研究中使用的其他蛋白质相比,含有更有效的免疫原性。这里提出的工作表明,生物信息学软件DNA星是分析蛋白质表位的有效工具,并且可用于优化蛋白质,该蛋白质可以诱导对 L的保护性免疫应答。 Pneumophila 。重组蛋白的交叉免疫,例如接头和Nlinker嵌合体,比单个蛋白质更高,产生更高的免疫。分发对象标识符http://dx.doi.org/10.1016/j.vaccine.2011.03.010

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