首页> 美国卫生研究院文献>PLoS Clinical Trials >One Dose of Staphylococcus aureus 4C-Staph Vaccine Formulated with a Novel TLR7-Dependent Adjuvant Rapidly Protects Mice through Antibodies, Effector CD4+ T Cells, and IL-17A
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One Dose of Staphylococcus aureus 4C-Staph Vaccine Formulated with a Novel TLR7-Dependent Adjuvant Rapidly Protects Mice through Antibodies, Effector CD4+ T Cells, and IL-17A

机译:一剂金黄色葡萄球菌4C-Staph疫苗与新型TLR7依赖性佐剂一起配制,可通过抗体,效应CD4 + T细胞和IL-17A快速保护小鼠

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摘要

A rapidly acting, single dose vaccine against Staphylococcus aureus would be highly beneficial for patients scheduled for major surgeries or in intensive care units. Here we show that one immunization with a multicomponent S. aureus candidate vaccine, 4C-Staph, formulated with a novel TLR7-dependent adjuvant, T7-alum, readily protected mice from death and from bacterial dissemination, both in kidney abscess and peritonitis models, outperforming alum-formulated vaccine. This increased efficacy was paralleled by higher vaccine-specific and α-hemolysin-neutralizing antibody titers and Th1/Th17 cell responses. Antibodies played a crucial protective role, as shown by the lack of protection of 4C-Staph/T7-alum vaccine in B-cell-deficient mice and by serum transfer experiments. Depletion of effector CD4+ T cells not only reduced survival but also increased S. aureus load in kidneys of mice immunized with 4C-Staph/T7-alum. The role of IL-17A in the control of bacterial dissemination in 4C-Staph/T7-alum vaccinated mice was indicated by in vivo neutralization experiments. We conclude that single dose 4C-Staph/T7-alum vaccine promptly and efficiently protected mice against S. aureus through the combined actions of antibodies, CD4+ effector T cells, and IL-17A. These data suggest that inclusion of an adjuvant that induces not only fast antibody responses but also IL-17-producing cell-mediated effector responses could efficaciously protect patients scheduled for major surgeries or in intensive care units.
机译:一种针对金黄色葡萄球菌的速效单剂疫苗对计划进行大手术或重症监护病房的患者非常有益。在这里,我们表明,在肾脏脓肿和腹膜炎模型中,用新型TLR7依赖性佐剂T7-alum配制的多组分金黄色葡萄球菌候选疫苗4C-Staph进行的免疫接种很容易保护小鼠免于死亡和细菌传播,优于明矾疫苗。这种更高的功效与更高的疫苗特异性抗体和α-溶血素中和抗体滴度以及Th1 / Th17细胞反应平行。抗体起着至关重要的保护作用,如缺乏B细胞的小鼠对4C-Staph / T7-alum疫苗缺乏保护以及血清转移实验所证明。用4C-Staph / T7-alum免疫的小鼠肾脏中效应CD4 + T细胞的耗竭不仅降低了存活率,而且增加了金黄色葡萄球菌的负荷。体内中和实验表明了IL-17A在4C-Staph / T7-alum疫苗接种小鼠中控制细菌传播的作用。我们得出的结论是,单剂量4C-Staph / T7-alum疫苗通过抗体,CD4 + 效应T细胞和IL-17A的联合作用迅速有效地保护了小鼠免受金黄色葡萄球菌的侵害。这些数据表明,包含不仅诱导快速抗体应答而且还诱导产生IL-17的细胞介导的效应子应答的佐剂可以有效地保护计划进行大手术或重症监护病房的患者。

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