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首页> 外文期刊>Immunology: An Official Journal of the British Society for Immunology >Humanized NOG mice as a model for tuberculosis vaccine-induced immunity: a comparative analysis with the mouse and guinea pig models of tuberculosis
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Humanized NOG mice as a model for tuberculosis vaccine-induced immunity: a comparative analysis with the mouse and guinea pig models of tuberculosis

机译:人源化的胭脂小鼠作为结核病疫苗诱导的免疫模型:具有结核病小鼠和豚鼠模型的对比分析

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摘要

The humanized mouse model has been developed as a model to identify and characterize human immune responses to human pathogens and has been used to better identify vaccine candidates. In the current studies, the humanized mouse was used to determine the ability of a vaccine to affect the immune response to infection with Mycobacterium tuberculosis. Both human CD4(+) and CD8(+) T cells responded to infection in humanized mice as a result of infection. In humanized mice vaccinated with either BCG or with CpG-C, a liposome-based formulation containing the M. tuberculosis antigen ESAT-6, both CD4 and CD8 T cells secreted cytokines that are known to be required for induction of protective immunity. In comparison to the C57BL/6 mouse model and Hartley guinea pig model of tuberculosis, data obtained from humanized mice complemented the data observed in the former models and provided further evidence that a vaccine can induce a human T-cell response. Humanized mice provide a crucial pre-clinical platform for evaluating human T-cell immune responses in vaccine development against M. tuberculosis.
机译:人源化的小鼠模型已被发展为识别和表征对人病原体的人类免疫反应的模型,并已用于更好地识别疫苗候选物。在目前的研究中,人源化的小鼠用于确定疫苗影响免疫应答对细胞分枝杆菌感染的能力。由于感染的结果,人CD4(+)和CD8(+)T细胞响应于人源化小鼠中的感染。在用BCG或CpG-C接种的人源化小鼠中,含有M.结核抗原ESAT-6的脂质体的制剂,CD4和CD8 T细胞的分泌细胞因子被称为诱导保护性免疫的细胞因子。与C57BL / 6小鼠模型和哈特利豚鼠模型的结核菌,从人源化小鼠获得的数据补充了前模型中观察到的数据,并提供了进一步证据,疫苗可以诱导人T细胞反应。人源化小鼠提供了评估疫苗发育中的人T细胞免疫反应的关键前平台,针对结核病。

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