首页> 外文期刊>The journal of immunology >A Recombinant G Protein Plus Cyclosporine A–Based Respiratory Syncytial Virus Vaccine Elicits Humoral and Regulatory T Cell Responses against Infection without Vaccine-Enhanced Disease
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A Recombinant G Protein Plus Cyclosporine A–Based Respiratory Syncytial Virus Vaccine Elicits Humoral and Regulatory T Cell Responses against Infection without Vaccine-Enhanced Disease

机译:重组G蛋白加基于环孢菌素A的呼吸道合胞病毒疫苗可引起体液和调节性T细胞应答,而无疫苗增强型疾病

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Respiratory syncytial virus (RSV) infection can cause severe disease in the lower respiratory tract of infants and older people. Vaccination with a formalin-inactivated RSV vaccine (FI-RSV) and subsequent RSV infection has led to mild to severe pneumonia with two deaths among vaccinees. The vaccine-enhanced disease (VED) was recently demonstrated to be due to an elevated level of Th2 cell responses following loss of regulatory T (Treg) cells from the lungs. To induce high levels of neutralizing Abs and minimize pathogenic T cell responses, we developed a novel strategy of immunizing animals with a recombinant RSV G protein together with cyclosporine A. This novel vaccine induced not only a higher level of neutralizing Abs against RSV infection, but, most importantly, also significantly higher levels of Treg cells that suppressed VED in the lung after RSV infection. The induced responses provided protection against RSV challenge with no sign of pneumonia or bronchitis. Treg cell production of IL-10 was one of the key factors to suppress VED. These finding indicate that G protein plus cyclosporine A could be a promising vaccine against RSV infection in children and older people.
机译:呼吸道合胞病毒(RSV)感染可导致婴儿和老年人下呼吸道的严重疾病。用福尔马林灭活的RSV疫苗(FI-RSV)进行的疫苗接种以及随后的RSV感染已导致轻度至重症肺炎,其中两例死亡。最近证明疫苗增强疾病(VED)是由于肺中调节性T(Treg)细胞丢失后Th2细胞反应水平升高所致。为了诱导高水平的中和抗体并最小化病原性T细胞应答,我们开发了一种用重组RSV G蛋白和环孢霉素A免疫动物的新策略。这种新型疫苗不仅诱导了更高水平的针对RSV感染的中和抗体,而且最重要的是,RSV感染后抑制肺VED的Treg细胞水平也显着升高。诱导的反应提供了针对RSV攻击的保护,没有肺炎或支气管炎的迹象。 IL-10的Treg细胞产生是抑制VED的关键因素之一。这些发现表明,G蛋白加环孢菌素A可能是针对儿童和老年人的RSV感染的有前途的疫苗。

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