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Protection against Respiratory Syncytial Virus Infection by DNA Immunization

机译:通过DNA免疫预防呼吸道合胞病毒感染

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摘要

Respiratory syncytial virus (RSV) remains a major cause of morbidity and mortality in infants and the elderly and is a continuing challenge for vaccine development. A murine T helper cell (Th) type 2 response associates with enhanced lung pathology, which has been observed in past infant trials using formalin-inactivated RSV vaccine. In this study, we have engineered an optimized plasmid DNA vector expressing the RSV fusion (F) protein (DNA-F). DNA-F was as effective as live RSV in mice at inducing neutralizing antibody and cytotoxic T lymphocyte responses, protection against infection, and high mRNA expression of lung interferon γ after viral challenge. Furthermore, a DNA-F boost could switch a preestablished anti-RSV Th2 response towards a Th1 response. Critical elements for the optimization of the plasmid constructs included expression of a secretory form of the F protein and the presence of the rabbit β-globin intron II sequence upstream of the F-encoding sequence. In addition, anti-F systemic immune response profile could be modulated by the route of DNA-F delivery: intramuscular immunization resulted in balanced responses, whereas intradermal immunization resulted in a Th2 type of response. Thus, DNA-F immunization may provide a novel and promising RSV vaccination strategy.
机译:呼吸道合胞病毒(RSV)仍然是婴儿和老年人发病和死亡的主要原因,也是疫苗开发的持续挑战。在过去的婴儿试验中,使用福尔马林灭活的RSV疫苗已经观察到了鼠T型辅助细胞(Th)2型应答与肺部病理改变有关。在这项研究中,我们设计了表达RSV融合(F)蛋白(DNA-F)的优化质粒DNA载体。在小鼠中,DNA-F在诱导中和抗体和细胞毒性T淋巴细胞反应,防止感染以及在病毒激发后肺干扰素γ的高mRNA表达方面与活RSV一样有效。此外,DNA-F增强可以将预先建立的抗RSV Th2反应切换为Th1反应。优化质粒构建体的关键因素包括表达F蛋白的分泌形式和在F编码序列上游的兔β-球蛋白内含子II序列的存在。此外,抗F全身免疫应答谱可通过DNA-F传递途径进行调节:肌内免疫可产生平衡应答,而皮内免疫可产生Th2型应答。因此,DNA-F免疫可以提供一种新颖且有希望的RSV疫苗接种策略。

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