首页> 美国卫生研究院文献>PLoS Pathogens >Relative Contribution of Th1 and Th17 Cells in Adaptive Immunity to Bordetella pertussis: Towards the Rational Design of an Improved Acellular Pertussis Vaccine
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Relative Contribution of Th1 and Th17 Cells in Adaptive Immunity to Bordetella pertussis: Towards the Rational Design of an Improved Acellular Pertussis Vaccine

机译:Th1和Th17细胞在适应性免疫中对百日咳博德特氏菌的相对贡献:改进的无细胞百日咳疫苗的合理设计。

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摘要

Whooping cough caused by Bordetella pertussis is a re-emerging infectious disease despite the introduction of safer acellular pertussis vaccines (Pa). One explanation for this is that Pa are less protective than the more reactogenic whole cell pertussis vaccines (Pw) that they replaced. Although Pa induce potent antibody responses, and protection has been found to be associated with high concentrations of circulating IgG against vaccine antigens, it has not been firmly established that host protection induced with this vaccine is mediated solely by humoral immunity. The aim of this study was to examine the relative contribution of Th1 and Th17 cells in host immunity to infection with B. pertussis and in immunity induced by immunization with Pw and Pa and to use this information to help rationally design a more effective Pa. Our findings demonstrate that Th1 and Th17 both function in protective immunity induced by infection with B. pertussis or immunization with Pw. In contrast, a current licensed Pa, administered with alum as the adjuvant, induced Th2 and Th17 cells, but weak Th1 responses. We found that IL-1 signalling played a central role in protective immunity induced with alum-adsorbed Pa and this was associated with the induction of Th17 cells. Pa generated strong antibody and Th2 responses, but was fully protective in IL-4-defective mice, suggesting that Th2 cells were dispensable. In contrast, Pa failed to confer protective immunity in IL-17A-defective mice. Bacterial clearance mediated by Pa-induced Th17 cells was associated with cell recruitment to the lungs after challenge. Finally, protective immunity induced by an experimental Pa could be enhanced by substituting alum with a TLR agonist that induces Th1 cells. Our findings demonstrate that alum promotes protective immunity through IL-1β-induced IL-17A production, but also reveal that optimum protection against B. pertussis requires induction of Th1, but not Th2 cells.
机译:尽管引入了更安全的脱细胞百日咳疫苗(Pa),但由百日咳博德特氏菌引起的百日咳却是一种新出现的传染病。对此的一种解释是,Pa比其替代的更具反应性的全细胞百日咳百日咳疫苗(Pw)缺乏保护性。尽管Pa诱导有效的抗体反应,并且发现与高浓度的针对疫苗抗原的循环IgG相关联,但尚未确定该疫苗诱导的宿主保护仅由体液免疫介导。这项研究的目的是检查Th1和Th17细胞在宿主免疫中对百日咳博德特氏菌感染以及Pw和Pa免疫诱导的免疫的相对贡献,并利用这些信息来合理设计更有效的Pa。研究结果表明,Th1和Th17均在百日咳博德特氏菌感染或Pw免疫诱导的保护性免疫中起作用。相比之下,目前许可的Pa(明矾作为佐剂)可诱导Th2和Th17细胞,但Th1反应较弱。我们发现,IL-1信号传导在铝吸附的Pa诱导的保护性免疫中起着核心作用,这与Th17细胞的诱导有关。 Pa产生强抗体和Th2反应,但在IL-4缺陷小鼠中具有完全保护作用,表明Th2细胞是可有可无的。相反,Pa未能在IL-17A缺陷小鼠中赋予保护性免疫。 Pa诱导的Th17细胞介导的细菌清除与细胞攻击后募集到肺部有关。最后,可以通过用诱导Th1细胞的TLR激动剂代替明矾来增强实验性Pa诱导的保护性免疫。我们的发现表明明矾可通过IL-1β诱导的IL-17A产生促进保护性免疫,但同时也表明,针对百日咳博德特氏菌的最佳保护作用需要诱导Th1细胞,而不诱导Th2细胞。

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