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Intranasal Boosting with an Adenovirus-Vectored Vaccine Markedly Enhances Protection by Parenteral Mycobacterium bovis BCG Immunization against Pulmonary Tuberculosis

机译:用腺病毒载体的疫苗进行鼻内加强治疗可显着增强肠胃外牛分枝杆菌BCG免疫接种对肺结核的保护作用。

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摘要

Parenterally administered Mycobacterium bovis BCG vaccine confers only limited immune protection from pulmonary tuberculosis in humans. There is a need for developing effective boosting vaccination strategies. We examined a heterologous prime-boost regimen utilizing BCG as a prime vaccine and our recently described adenoviral vector expressing Ag85A (AdAg85A) as a boost vaccine. Since we recently demonstrated that a single intranasal but not intramuscular immunization with AdAg85A was able to induce potent protection from pulmonary Mycobacterium tuberculosis challenge in a mouse model, we compared the protective effects of parenteral and mucosal booster immunizations following subcutaneous BCG priming. Protection by BCG prime immunization was not effectively boosted by subcutaneous BCG or intramuscular AdAg85A. In contrast, protection by BCG priming was remarkably boosted by intranasal AdAg85A. Such enhanced protection by intranasal AdAg85A was correlated to the numbers of gamma interferon-positive CD4 and CD8 T cells residing in the airway lumen of the lung. Our study demonstrates that intranasal administration of AdAg85A represents an effective way to boost immune protection by parenteral BCG vaccination.
机译:肠胃外施用的牛分枝杆菌卡介苗疫苗只能对人类的肺结核提供有限的免疫保护。需要开发有效的加强疫苗接种策略。我们研究了利用BCG作为主要疫苗的异源加强免疫方案,以及我们最近描述的表达Ag85A(AdAg85A)的腺病毒载体作为加强疫苗。由于我们最近证明在小鼠模型中用AdAg85A进行单次鼻内而非肌肉内免疫能够诱导针对肺结核分枝杆菌攻击的有效保护,因此我们比较了皮下BCG灌注后肠胃外和粘膜加强免疫的保护作用。皮下BCG或肌内AdAg85A不能有效增强BCG初次免疫的保护作用。相反,鼻内AdAg85A显着增强了BCG引发的保护作用。鼻内AdAg85A的这种增强的保护作用与肺气道内腔中γ干扰素阳性CD4和CD8 T细胞的数量有关。我们的研究表明,鼻腔内施用AdAg85A代表通过肠胃外BCG疫苗接种增强免疫保护的有效方法。

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