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首页> 外文期刊>The Journal of investigative dermatology. >Local ultraviolet B irradiation impairs contact hypersensitivity induction by triggering release of tumor necrosis factor-alpha from mast cells. Involvement of mast cells and Langerhans cells in susceptibility to ultraviolet B.
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Local ultraviolet B irradiation impairs contact hypersensitivity induction by triggering release of tumor necrosis factor-alpha from mast cells. Involvement of mast cells and Langerhans cells in susceptibility to ultraviolet B.

机译:局部紫外线B辐射通过触发从肥大细胞释放肿瘤坏死因子α来削弱接触超敏反应的诱导作用。肥大细胞和朗格汉斯细胞参与对紫外线B的敏感性。

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Our laboratory has previously demonstrated that ultraviolet B radiation impairs contact hypersensitivity induction in ultraviolet B susceptible mice through a tumor necrosis factor-alpha-dependent mechanism, involving calcitonin gene related peptide and cutaneous mast cells. This study was designed to test directly whether mast cells are the source of tumor necrosis factor-alpha, to account for the ultra-violet B-susceptible phenotype. As dermal mast cells seem to release tumor necrosis factor-alpha following exposure to ultraviolet B, we investigated whether tumor necrosis factor-alpha released by mast cells could mediate impairment of contact hypersensitivity in a manner similar to that found with ultraviolet B radiation treatment. First, we loaded Fcepsilon receptors of mast cells of ultraviolet B-susceptible (C3H/HeN), ultraviolet B-resistant (C3H/HeJ), and mast-cell deficient (Sl/Sld) mice by intradermal injections of anti-dinitrophenyl immunoglobulin E antibodies. Twenty-four hours later, dinitrophenyl was injected intravenously, and within 30 min oxazolone was painted on injected skin sites. Contact hypersensitivity induction was impaired in ultraviolet B-susceptible mice, but not in ultraviolet B-resistant or Sl/Sld mice, and treatment with anti-tumor necrosis factor-alpha antibodies was able to reverse this impairment of contact hypersensitivity. Second, we have found that ultraviolet B radiation did not impair contact hypersensitivity induction when haptens were painted on irradiated skin of mast cell deficient mice. As ultraviolet B radiation impairs contact hypersensitivity induction through a tumor necrosis factor-alpha-dependent mechanism, we conclude that ultraviolet B radiation triggers the prompt release of tumor necrosis factor-alpha from dermal mast cells, and that mast cell-derived tumor necrosis factor-alpha interferes with generation of the hapten-specific signal required for contact hypersensitivity induction. In addition, we are providing data that indicate that tumor necrosis factor-alpha levels released from mast cells as well as sensitivity of Langerhans cells to tumor necrosis factor-alpha contribute in defining the phenotypes of resistance versus sensitivity to ultra-violet B radiation.
机译:我们的实验室以前已经证明,紫外线B辐射通过肿瘤坏死因子-α依赖性机制(包括降钙素基因相关肽和皮肤肥大细胞)损害了对紫外线B易感小鼠的超敏反应。这项研究旨在直接测试肥大细胞是否是肿瘤坏死因子-α的来源,以解释紫外线B敏感表型。由于皮肤肥大细胞在暴露于紫外线B后似乎会释放肿瘤坏死因子-α,因此我们研究了肥大细胞释放的肿瘤坏死因子-α是否可以以类似于紫外线B辐射治疗的方式介导接触性超敏反应的损害。首先,我们通过皮内注射抗二硝基苯基免疫球蛋白E加载了对紫外线B敏感(C3H / HeN),对紫外线B抗性(C3H / HeJ)和肥大细胞缺乏(S1 / Sld)小鼠的肥大细胞的Fcepsilon受体抗体。二十四小时后,静脉内注射二硝基苯,并在30分钟内将恶唑酮涂在注射的皮肤部位。在对紫外线B敏感的小鼠中,接触超敏反应的诱导受损,但对抗紫外线B的Sl / Sld小鼠则没有,并且用抗肿瘤坏死因子-α抗体治疗能够逆转这种接触超敏反应的损害。第二,我们发现当将半抗原涂在肥大细胞缺陷小鼠的受辐照皮肤上时,紫外线B辐射不会损害接触超敏反应的诱导。由于紫外线B辐射通过肿瘤坏死因子-α依赖性机制削弱了接触超敏反应的诱导,因此我们得出结论,紫外线B辐射触发了从皮肤肥大细胞中迅速释放肿瘤坏死因子-α,以及肥大细胞衍生的肿瘤坏死因子- α干扰了接触超敏反应诱导所需的半抗原特异性信号的产生。此外,我们提供的数据表明,肥大细胞释放的肿瘤坏死因子-α水平以及朗格汉斯细胞对肿瘤坏死因子-α的敏感性有助于确定抗性表型与对紫外线B辐射的敏感性。

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