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A Heterologous DNA Priming-Mycobacterium bovis BCG Boosting Immunization Strategy Using Mycobacterial Hsp70, Hsp65, and Apa Antigens Improves Protection against Tuberculosis in Mice

机译:使用分枝杆菌Hsp70,Hsp65和Apa抗原的异源DNA启动牛牛分枝杆菌BCG增强免疫策略可提高对小鼠结核病的保护

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Tuberculosis is responsible for >2 million deaths a year, and the number of new cases is rising worldwide. DNA vaccination combined with Mycobacterium bovis bacillus Calmette Guérin (BCG) represents a potential strategy for prevention of this disease. Here, we used a heterologous prime-boost immunization approach using a combination of DNA plasmids and BCG in order to improve the efficacy of vaccination against Mycobacterium tuberculosis infection in mice. As model antigens, we selected the M. tuberculosis Apa (for alanine-proline-rich antigen) and the immunodominant Hsp65 and Hsp70 mycobacterial antigens combined with BCG. We demonstrated that animals injected with a combination of DNA vectors expressing these antigens, when boosted with BCG, showed increased specific antimycobacterial immune responses compared to animals vaccinated with BCG alone. More importantly, the protection achieved with this regimen was also significantly better than with BCG alone.
机译:结核病每年导致超过200万人死亡,全球范围内新病例的数量正在增加。 DNA疫苗与牛分枝杆菌卡门特·格林(BCG)的结合代表了一种预防这种疾病的潜在策略。在这里,我们使用了结合了DNA质粒和BCG的异源初免-加强免疫方法,以提高针对小鼠结核分枝杆菌感染的疫苗接种效果。作为模型抗原,我们选择了 M。结核Apa(富含丙氨酸和脯氨酸的抗原)和免疫优势的Hsp65和Hsp70分枝杆菌抗原与卡介苗结合。我们证明,与单独接种BCG的动物相比,注射有BCG增强表达这些抗原的DNA载体的动物注射的动物表现出更高的特异性抗分枝杆菌免疫反应。更重要的是,与单独使用BCG相比,通过该方案获得的保护效果也明显更好。

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