紫外线通过减少效应性 CD4 T 细胞抑制小鼠过敏性气道疾病。

UV inhibits allergic airways disease in mice by reducing effector CD4 T cells.

机构信息

Telethon Institute for Child Health Research and Centre for Child Health Research, The University of Western Australia, West Perth, Western Australia, Australia.

出版信息

Clin Exp Allergy. 2010 May;40(5):772-85. doi: 10.1111/j.1365-2222.2010.03469.x. Epub 2010 Mar 4.

DOI:10.1111/j.1365-2222.2010.03469.x

PMID:20214669

Abstract

BACKGROUND

In human asthma, and experimental allergic airways disease in mice, antigen-presenting cells and CD4(+) effector cells at the airway mucosa orchestrate, and CD4(+)CD25(+) regulatory T cells attenuate, allergen immunity. UV irradiation of skin before sensitization with ovalbumin (OVA) causes significantly reduced asthma-like responses in respiratory tissues.

OBJECTIVE

To determine whether UV-induced changes in CD11c(+) cells, CD4(+)CD25(+) effector cells or CD4(+)CD25(+) regulatory cells in the trachea and airway draining lymph nodes (ADLNs) were responsible for reduced allergic airways disease.

METHODS

The phenotype and function of CD11c(+) cells and CD4(+)CD25(+) cells in the trachea and ADLNs of UV- and non-irradiated, OVA-sensitized mice was examined 24 h after a single exposure to aerosolized OVA.

RESULTS

No changes in the function of CD11c(+) cells from UV-irradiated mice were observed. CD4(+)CD25(+) cells from UV-irradiated, OVA-sensitized mice harvested 24 h after OVA aerosol proliferated less in response to OVA in vitro and were unable to suppress the proliferation of OVA-sensitized responder cells. This result suggested reduced activation of effector T cells in the airway mucosa of UV-irradiated, OVA-sensitized mice. To exclude regulatory cells of any type, there was similar proliferation in vivo to aerosolized OVA by CFSE-loaded, OVA-TCR-specific CD4(+) cells adoptively transferred into UV- and non-irradiated, OVA-sensitized mice. In addition, there was no difference in the expression of regulatory T cell markers (Foxp3, IL-10, TGF-beta mRNA). To examine effector T cells, ADLN cells from UV-irradiated, OVA-sensitized and -challenged mice were cultured with OVA. There was reduced expression of the early activation marker CD69 by CD4(+)CD25(+) cells, and reduced proliferation in the absence of the regulatory cytokine, IL-10.

CONCLUSION

Reduced allergic airways disease in UV-irradiated mice is due to fewer effector CD4(+)CD25(+) cells in the trachea and ADLNs, and not due to UV-induced regulatory cells.

摘要

背景

在人类哮喘和实验性变应性气道疾病中，气道黏膜中的抗原呈递细胞和 CD4+效应细胞协调变应原免疫，而 CD4+CD25+调节性 T 细胞则减弱变应原免疫。在致敏前用卵清蛋白（OVA）进行皮肤紫外线照射会导致呼吸道组织中哮喘样反应明显减少。

目的

确定气管和引流淋巴结（ADLN）中 CD11c+细胞、CD4+CD25+效应细胞或 CD4+CD25+调节细胞的紫外线诱导变化是否导致过敏性气道疾病减少。

方法

在单次雾化 OVA 暴露后 24 小时，检查 UV 和非照射、OVA 致敏小鼠气管和 ADLN 中 CD11c+细胞和 CD4+CD25+细胞的表型和功能。

结果

未观察到来自 UV 照射小鼠的 CD11c+细胞功能发生变化。OVA 雾化后 24 小时从 UV 照射、OVA 致敏的小鼠中收获的 CD4+CD25+细胞对 OVA 的体外增殖减少，并且不能抑制 OVA 致敏反应细胞的增殖。这一结果表明，UV 照射的 OVA 致敏小鼠气道黏膜中的效应 T 细胞激活减少。为排除任何类型的调节细胞，将 CFSE 加载的、OVA-TCR 特异性 CD4+细胞过继转移到 UV 和非照射、OVA 致敏的小鼠中，这些细胞对雾化 OVA 的体内增殖相似。此外，调节性 T 细胞标志物（Foxp3、IL-10、TGF-βmRNA）的表达没有差异。为了检查效应 T 细胞，从 UV 照射、OVA 致敏和 challenged 的小鼠的 ADLN 细胞中用 OVA 培养。CD4+CD25+细胞中早期激活标记物 CD69 的表达减少，在缺乏调节细胞因子 IL-10 的情况下增殖减少。