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首页> 外文期刊>Clinical and vaccine immunology: CVI >Investigating the Induction of Vaccine-Induced Th17 and Regulatory T Cells in Healthy, Mycobacterium bovis BCG-Immunized Adults Vaccinated with a New Tuberculosis Vaccine, MVA85A
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Investigating the Induction of Vaccine-Induced Th17 and Regulatory T Cells in Healthy, Mycobacterium bovis BCG-Immunized Adults Vaccinated with a New Tuberculosis Vaccine, MVA85A

机译:研究在牛分枝杆菌BCG免疫的健康成年人中接种新的结核疫苗MVA85A的疫苗诱导的Th17和调节性T细胞的诱导

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Tuberculosis (TB) remains a threat to global health. While advances in diagnostics and treatment are crucial to the containment of the epidemic, it is likely that elimination of the disease can only be achieved through vaccination. Vaccine-induced protection from Mycobacterium tuberculosis is dependent, at least in part, on a robust Th1 response, yet little is known of the ability of TB vaccines to induce other T-cell subsets which may influence vaccine efficacy. Interleukin-17A (IL-17A) is a proinflammatory cytokine produced by Th17 cells which has been associated with both immune pathology and protection against infectious disease. Following vaccination with MVA85A, a viral vector vaccine aimed at enhancing immune responses to M. tuberculosis, antigen-specific IL-17A-producing T cells were induced in the peripheral blood of healthy volunteers. These T cells are detected later than gamma interferon (IFN-γ)-secreting T cells and are of a low magnitude. Preexisting immune responses to mycobacterial antigens were associated with higher CD4+ CD25hi CD39+ T-cell levels in the periphery and a reduced capacity to produce IL-17A following immunization. These data highlight the intricate balance of effector and regulatory immune responses induced by vaccination and that preexisting immunity to mycobacterial antigens may affect the composition of vaccine-induced T-cell subsets.
机译:结核病(TB)仍然威胁着全球健康。尽管诊断和治疗的进步对于控制这一流行病至关紧要,但疾病的消除可能只能通过接种疫苗来实现。疫苗对结核分枝杆菌的保护至少部分取决于强大的Th1反应,但对于结核病疫苗诱导其他可能影响疫苗功效的T细胞亚群的能力知之甚少。白细胞介素17A(IL-17A)是由Th17细胞产生的促炎细胞因子,与免疫病理学和传染病防护有关。用MVA85A疫苗接种后,病毒载体疫苗旨在增强对 M的免疫应答。在健康志愿者的外周血中诱导了结核病,产生抗原的IL-17A T细胞。这些T细胞的检测时间要晚于分泌γ-干扰素(IFN-γ)的T细胞,并且它们的幅度很小。先前对分枝杆菌抗原的免疫反应与外周CD4 + CD25 hi CD39 + T细胞水平升高和生产能力降低有关免疫后IL-17A。这些数据突显了疫苗诱导的效应子和调节性免疫反应之间的复杂平衡,对分枝杆菌抗原的预先存在的免疫力可能会影响疫苗诱导的T细胞亚群的组成。

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