首页> 美国卫生研究院文献>Immunology >Regulation of delayed-type hypersensitivity-like responses in the mouse lung determined with histological procedures: serotonin T-cell suppressor-inducer factor and high antigen dose tolerance regulate the magnitude of T-cell dependent inflammatory reactions.
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Regulation of delayed-type hypersensitivity-like responses in the mouse lung determined with histological procedures: serotonin T-cell suppressor-inducer factor and high antigen dose tolerance regulate the magnitude of T-cell dependent inflammatory reactions.

机译:调节小鼠肺部迟发型超敏反应样反应的方法是通过组织学方法确定的:5-羟色胺T细胞抑制因子和高抗原剂量耐受性可调节T细胞依赖性炎症反应的程度。

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摘要

We have studied delayed-type hypersensitivity (DTH) responses to picryl chloride (PCl) in the lungs of mice. Intranasal challenge with 0.6% picryl sulphonic acid (PSA), a water soluble form of PCl, of BALB/c mice, sensitized with PCl epicutaneously 1 week earlier, induced an accumulation of mononuclear inflammatory cells around bronchioli and blood vessels. Maximal inflammatory responses were seen 48 hr after challenge. These responses were antigen-specific, and also T-cell dependent, since athymic nude mice failed to show this reaction. A role for mast cells in the responses was studied using two strains of mast cell-deficient mice. In one of these (W/Wv) lung DTH responses to PCl were reduced severely. In the other strain (S1/S1d) the responses around vessels were decreased slightly, whereas the responses in the interstitial tissue and around bronchioli were similar to those in +/+ littermate controls. Involvement of serotonin was investigated using two serotonin receptor antagonists, i.e. methysergide and ketanserin. Treatment of mice with either of the antagonists prevented occurrence of the DTH-like reaction in the lung after intranasal antigen challenge. In the lungs of sensitized mice, significantly increased permeability was established 2 hr after antigen challenge. It was concluded that release of serotonin in the lung may provide an environment that comprises local vascular permeability and that facilitates the local recruitment and possibly the activation of DTH effector T cells, leading to subsequent attraction of mononuclear leucocytes into the lung. Immunological regulation of the DTH-like reactions in the lung was similar to that of contact sensitivity in the skin, since intravenous injection of an antigen-specific T-cell suppressor inducer factor prior to sensitization or pretreatment with a high dose of picryl sulphonic acid intravenously both resulted in reduction of the DTH-like lung histological response to picryl sulphonic acid. From these findings it was concluded that DTH-like lung responses are similar to DTH responses in the skin.
机译:我们已经研究了小鼠肺中对氯化苦基吡啶(PCl)的迟发型超敏反应(DTH)。用0.6%苦味素磺酸(PSA)(一种PC1的水溶性形式)对BALB / c小鼠进行鼻内攻击,在1周前经表皮对PC1致敏,诱导了细支气管和血管周围的单核炎性细胞积聚。攻击后48小时观察到最大的炎症反应。这些反应是抗原特异性的,并且也是T细胞依赖性的,因为无胸腺裸鼠不能显示该反应。使用两种缺乏肥大细胞的小鼠研究了肥大细胞在反应中的作用。在这些(W / Wv)之一中,肺对PC1的DTH反应严重降低。在其他菌株(S1 / S1d)中,血管周围的反应略有降低,而间质组织和细支气管周围的反应与+ / +同窝对照的反应相似。使用两种5-羟色胺受体拮抗剂,即美塞麦肽和酮色林,研究了5-羟色胺的参与。用任一种拮抗剂治疗小鼠都可防止鼻内抗原攻击后肺中发生DTH样反应。在致敏小鼠的肺中,抗原攻击后2小时建立了明显的通透性。结论是5-羟色胺在肺中的释放可以提供包括局部血管通透性的环境,并促进局部募集和可能的DTH效应T细胞活化,从而导致单核白细胞随后吸引到肺中。肺部DTH样反应的免疫学调节与皮肤接触敏感性的免疫学调节相似,因为在致敏或用高剂量苦味素磺酸静脉内预处理之前静脉注射抗原特异性T细胞抑制因子两者均导致对苦瓜磺酸的DTH样肺组织学反应降低。从这些发现可以得出结论,DTH样肺反应类似于皮肤中的DTH反应。

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