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Adjuvantic cytokine IL-33 improves the protective immunity of cocktailed DNA vaccine of ROP5 and ROP18 against toxoplasma gondii infection in mice

机译:辅助细胞因子IL-33改善了ROP5和ROP18的鸡尾酒DNA疫苗的保护性免疫,对小鼠的弓形虫感染

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摘要

Toxoplasma gondii is a threat for immunocompromized individuals, and no treatment is available for enhancing immunity against infection. Molecular adjuvants may improve the efficacy of DNA vaccine-induced T cell immunity. Here, we report that cocktailed DNA immunization with ROP5 and ROP18 boosted immune responses induced by a single DNA immunization with ROP5 or ROP18, but also that co-administration of molecular adjuvant IL-33 enhanced immune efficacy induced by this cocktailed DNA vaccination. These improved immune responses were characterized by higher Toxoplasma-specific IgG2a titers, Th1 responses associated with the production of IFN-γ, IL-2, IL-12, as well as cell-mediated activity with higher frequencies of CD8+ and CD4+ T cells. More importantly, this enhanced immunity has the ability to confer remarkable protection against a high dose lethal challenge of the T. gondii RH strain and thus against chronic infection with the T. gondii PRU strain. These data show that IL-33 is a promising immunoadjuvant to facilitate humoral as well as cellular immunity in a vaccine setting against T. gondii, and suggest that it should be evaluated in strategies against other apicomplexan parasites.
机译:弓形虫是免疫受损个体的威胁,没有治疗可增强抗感染的免疫力。分子佐剂可以提高DNA疫苗诱导的T细胞免疫的功效。在这里,我们报告,与ROP5和ROP18鸡尾酒会DNA免疫升压用ROP5或ROP18单个DNA免疫诱导的免疫应答,而且还由这个鸡尾酒会DNA疫苗接种诱导的分子佐剂IL-33增强的免疫效能的共同给药。通过更高弓形虫-特异性IgG2a效价这些改进的免疫应答,其特征在于,具有生产IFN-γ的,IL-2,IL-12,以及细胞介导的活性与CD8 +和CD4 + T细胞的更高的频率相关联的Th1应答。更重要的是,这个增强的免疫力有赋予对抗弓形虫RH株的高剂量致死攻击针对慢性感染显着的保护,并因此与刚地弓形虫PRU应变的能力。这些数据表明,IL-33是一种很有前途的免疫佐剂,以促进体液以及在对弓形虫疫苗设置细胞免疫,并建议应在对其他顶复门寄生虫的战略进行评估。

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