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首页> 外文期刊>Vaccine >The use of Th1 cytokines, IL-12 and IL-23, to modulate the immune response raised to a DNA vaccine delivered by gene gun
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The use of Th1 cytokines, IL-12 and IL-23, to modulate the immune response raised to a DNA vaccine delivered by gene gun

机译:使用Th1细胞因子IL-12和IL-23调节对基因枪传递的DNA疫苗产生的免疫反应

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摘要

Unlike intramuscular injection, gene gun delivery of DNA drives a strong type 2 response. In an effort to counter this, we have genetically fused the type 1 cytokines, IL-12 and IL-23, to the hemagglutinin (HA) gene from influenza APR/8/34, and delivered these DNA constructs to Balb/c mice. Gene gun delivery of the HA gene was able to induce antibody production by all vaccinated mice. Linking of IL-12 caused almost complete suppression of immune responses whereas mice vaccinated with IL-23HA showed long-lived IgG1 antibody levels. Splenocytes from IL-23HA vaccinated mice also tended to produce more IL-5 and IFNgamma after restimulation in vitro than splenocytes from HA vaccinated mice. While codelivery of IL-23 did not change the type of immune response it may increase its longevity following vaccination.
机译:与肌肉注射不同,DNA的基因枪传递可驱动强烈的2型反应。为了解决这个问题,我们将1型细胞因子IL-12和IL-23与流感APR / 8/34的血凝素(HA)基因进行了基因融合,并将这些DNA构建体交付给Balb / c小鼠。 HA基因的基因枪递送能够诱导所有接种疫苗的小鼠产生抗体。 IL-12的连接几乎完全抑制了免疫反应,而接种IL-23HA的小鼠表现出长寿命的IgG1抗体水平。与来自HA疫苗的小鼠的脾细胞相比,来自IL-23HA疫苗的小鼠的脾细胞在体外再刺激后也倾向于产生更多的IL-5和IFNgamma。虽然IL-23的代码传递并没有改变免疫应答的类型,但在接种疫苗后可能会延长其寿命。

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