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Investigation of Functional Activity of Cells in Granulomatous Inflammatory Lesions from Mice with Latent Tuberculous Infection in the New Ex Vivo Model

机译:新的体内模型对潜伏性结核感染小鼠肉芽肿性炎性病变中细胞功能活性的研究

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The new ex vivo model system measuring functional input of individual granuloma cells to formation of granulomatous inflammatory lesions in mice with latent tuberculous infection has been developed and described in the current study. Monolayer cultures of cells that migrated from individual granulomas were established in the proposed culture settings for mouse spleen and lung granulomas induced by in vivo exposure to BCG vaccine. The cellular composition of individual granulomas was analyzed. The expression of the leukocyte surface markers such as phagocytic receptors CD11b, CD11c, CD14, and CD16/CD32 and the expression of the costimulatory molecules CD80, CD83, and CD86 were tested as well as the production of proinflammatory cytokines (IFNγ and IL-1α) and growth factors (GM-CSF and FGFb) for cells of individual granulomas. The colocalization of the phagocytic receptors and costimulatory molecules in the surface microdomains of granuloma cells (with and without acid-fast BCG-mycobacteria) has also been detected. It was found that some part of cytokine macrophage producers have carried acid-fast mycobacteria. Detected modulation in dynamics of production of pro-inflammatory cytokines, growth factors, and leukocyte surface markers by granuloma cells has indicated continued processes of activation and deactivation of granuloma inflammation cells during the latent tuberculous infection progress in mice.
机译:在当前的研究中已经开发并描述了新的离体模型系统,该系统可测量单个肉芽肿细胞功能输入到潜伏性结核感染小鼠中肉芽肿性炎症病变的形成。在拟议的培养环境中,通过体内暴露于BCG疫苗诱导的小鼠脾脏和肺肉芽肿,建立了从单个肉芽肿迁移的细胞的单层培养。分析了各个肉芽肿的细胞组成。测试了白细胞表面标记(如吞噬受体CD11b,CD11c,CD14和CD16 / CD32)的表达以及共刺激分子CD80,CD83和CD86的表达,以及促炎细胞因子(IFNγ和IL-1α)的产生。 )和单个肉芽肿细胞的生长因子(GM-CSF和FGFb)。吞噬细胞受体和共刺激分子在肉芽肿细胞(有和没有抗酸的BCG分枝杆菌)的表面微区中的共定位也已被检测到。发现细胞因子巨噬细胞生产者的某些部分携带抗酸分枝杆菌。肉芽肿细胞检测到促炎性细胞因子,生长因子和白细胞表面标志物产生动力学的调节表明,在小鼠潜伏性结核感染过程中,肉芽肿炎症细胞的激活和失活过程持续进行。

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