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首页> 外文期刊>Clinical and vaccine immunology: CVI >Using Data from Macaques To Predict Gamma Interferon Responses after Mycobacterium bovis BCG Vaccination in Humans: a Proof-of-Concept Study of Immunostimulation/Immunodynamic Modeling Methods
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Using Data from Macaques To Predict Gamma Interferon Responses after Mycobacterium bovis BCG Vaccination in Humans: a Proof-of-Concept Study of Immunostimulation/Immunodynamic Modeling Methods

机译:使用数据从猕猴预测γ牛结核分枝杆菌后干扰素反应接种卡介苗疫苗在人类:一个概念验证研究Immunostimulation / Immunodynamic建模方法

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Macaques play a central role in the development of human tuberculosis (TB) vaccines. Immune and challenge responses differ across macaque and human subpopulations. We used novel immunostimulation/immunodynamic modeling methods in a proof-of-concept study to determine which macaque subpopulations best predicted immune responses in different human subpopulations. Data on gamma interferon (IFN-gamma)-secreting CD4(+) T cells over time after recent Mycobacterium bovis BCG vaccination were available for 55 humans and 81 macaques. Human population covariates were baseline BCG vaccination status, time since BCG vaccination, gender, and the monocyte/lymphocyte cell count ratio. The macaque population covariate was the colony of origin. A two-compartment mathematical model describing the dynamics of the IFN-gamma T cell response after BCG vaccination was calibrated to these data using nonlinear mixed-effects methods. The model was calibrated to macaque and human data separately. The association between subpopulations and the BCG immune response in each species was assessed. The macaque subpopulations that best predicted immune responses in different human subpopulations were identified using Bayesian information criteria. We found that the macaque colony and the human baseline BCG status were significantly (P < 0.05) associated with the BCG-induced immune response. For humans who were BCG naive at baseline, Indonesian cynomolgus macaques and Indian rhesus macaques best predicted the immune response. For humans who had already been BCG vaccinated at baseline, Mauritian cynomolgus macaques best predicted the immune response. This work suggests that the immune responses of different human populations may be best modeled by different macaque colonies, and it demonstrates the potential utility of immunostimulation/immunodynamic modeling to accelerate TB vaccine development.
机译:猕猴的发展中发挥核心作用人类结核病疫苗。在猕猴和挑战的反应不同人类的亚种。immunostimulation / immunodynamic建模方法在一个概念验证研究,以确定哪些猕猴种群最好预测免疫反应在不同的人类亚种。γ干扰素(IFN-gamma)分泌CD4 (+)最近的分枝杆菌后随时间T细胞宝BCG接种5581年人类和猕猴。接种卡介苗是基线状态,反是;BCG疫苗接种以来,性别,和单核细胞和淋巴细胞细胞计数率。协变量是人口群的起源。两舱制描述的数学模型IFN-gamma T细胞反应的动力学卡介苗接种是这些数据校准使用非线性mixed-effects方法。被校准猕猴和人类数据分开。亚种群和BCG免疫反应每一个物种被评估。亚种群最能预测免疫反应在不同的人类种群确定使用贝叶斯信息准则。我们发现猕猴和人类殖民地基线BCG地位显著(P < 0.05)与BCG-induced免疫反应有关。对人类BCG天真的基线,印尼猕猴猕猴和印度的恒河猕猴最佳预测免疫应答。人类已经BCG接种疫苗基线,毛里求斯的猕猴猕猴最好预测了免疫反应。不同人类的免疫反应人口可能最好由不同的建模猕猴殖民地,它展示了的潜在效用immunostimulation / immunodynamic建模加速结核病疫苗的发展。

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