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Single Mucosal, but Not Parenteral, Immunization with Recombinant Adenoviral-Based Vaccine Provides Potent Protection from Pulmonary Tuberculosis

机译:重组腺病毒疫苗对单个粘膜而非肠胃外的免疫提供了有效的保护,以预防肺结核

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Bacillus Calmette-Guérin (BCG) vaccine has failed to control the global tuberculosis (TB) epidemic, and there is a lack of safe and effective mucosal vaccines capable of potent protection against pulmonary TB. A recombinant replication-deficient adenoviral-based vaccine expressing an immunogenic Mycobacterium tuberculosis Ag Ag85A (AdAg85A) was engineered and evaluated for its potential to be used as a respiratory mucosal TB vaccine in a murine model of pulmonary TB. A single intranasal, but not i.m., immunization with AdAg85A provided potent protection against airway Mycobacterium tuberculosis challenge at an improved level over that by cutaneous BCG vaccination. Systemic priming with an Ag85A DNA vaccine and mucosal boosting with AdAg85A conferred a further enhanced immune protection which was remarkably better than BCG vaccination. Such superior protection triggered by AdAg85 mucosal immunization was correlated with much greater retention of Ag-specific T cells, particularly CD4 T cells, in the lung and was shown to be mediated by both CD4 and CD8 T cells. Thus, adenoviral TB vaccine represents a promising novel vaccine platform capable of potent mucosal immune protection against TB. Our study also lends strong evidence that respiratory mucosal vaccination is critically advantageous over systemic routes of vaccination against TB.
机译:卡介苗芽孢杆菌(BCG)疫苗未能控制全球结核病(TB)的流行,并且缺乏能够有效保护肺结核的安全有效的粘膜疫苗。表达一种免疫原性结核分枝杆菌Ag Ag85A(AdAg85A)的重组复制缺陷型腺病毒疫苗进行了工程设计,并评估了其在肺结核鼠模型中用作呼吸道粘膜TB疫苗的潜力。用AdAg85A进行的一次鼻内免疫接种(但不是i.m.)提供了有效的抗气管结核分枝杆菌攻击的保护,其保护水平高于皮肤BCG疫苗接种。用Ag85A DNA疫苗全身性引发和用AdAg85A进行粘膜加强免疫后,免疫保护作用进一步增强,这明显优于BCG疫苗接种。由AdAg85粘膜免疫引发的这种优越的保护作用与Ag特异性T细胞(特别是CD4 T细胞)在肺中的保留更大有关,并且被CD4和CD8 T细胞介导。因此,腺病毒结核病疫苗代表了一种有希望的新型疫苗平台,能够针对结核病进行有效的粘膜免疫保护。我们的研究还提供了强有力的证据,证明呼吸道粘膜疫苗接种比针对结核病的全身疫苗接种途径至关重要。

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