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经接触性致敏剂处理的角质形成细胞对小鼠表皮TCR-γδ⁺ T细胞的激活作用。

Activation of murine epidermal TCR-gamma delta+ T cells by keratinocytes treated with contact sensitizers.

作者信息

Huber H, Descossy P, van Brandwijk R, Knop J

机构信息

Department of Dermatology, Johannes Gutenberg University, Mainz, Germany.

出版信息

J Immunol. 1995 Sep 15;155(6):2888-94.

PMID:7673705
Abstract

The vast majority of TCR gamma delta+, CD4-, CD8- T cells resident in the adult mouse epidermis expresses tissue-specific V-region genes (V gamma 3/V delta 1) in the absence of junctional diversity. The role this unique T cell population plays in the immune surveillance of the skin is not clear. It has been shown that dendritic epidermal T cells (DETC) were activated by stressed keratinocytes and that stimulated DETC produced, for example, a keratinocyte-specific growth factor. To investigate whether DETC are involved in the induction of a contact allergy, we examined the influence of contact sensitizers and nonsensitizing contact irritants on the DETC response toward epidermal symbionts. We show that 9 of 15 cloned DETC are specifically activated, apparently in a non-MHC-restricted way, to proliferate in the presence of keratinocytes or unseparated epidermal cells, which were treated with a sensitizing agent either in vivo or in vitro. All seven tested contact sensitizing substances activated all of the reactive DETC, while keratinocytes/epidermal cells treated with nonsensitizing irritants were as nonstimulatory as vehicle controls. We demonstrate that direct cell to cell contact of DETC and stimulatory keratinocytes/epidermal cells was required and that the TCR was involved in the induction of DETC proliferation. This specific reactivity of DETC toward keratinocytes or epidermal cells pretreated with a contact sensitizer may be indicative of participation of epidermal T cells in the induction of a contact sensitivity and points to a possible role of DETC in the skin immune system.

摘要

成年小鼠表皮中绝大多数驻留的TCRγδ⁺、CD4⁻、CD8⁻ T细胞在缺乏连接多样性的情况下表达组织特异性V区基因(Vγ3/Vδ1)。这一独特的T细胞群体在皮肤免疫监视中所起的作用尚不清楚。已有研究表明,树突状表皮T细胞(DETC)可被应激的角质形成细胞激活,且被激活的DETC会产生例如角质形成细胞特异性生长因子。为了研究DETC是否参与接触性过敏的诱导,我们检测了接触性致敏剂和非致敏性接触性刺激物对DETC针对表皮共生菌反应的影响。我们发现,15个克隆的DETC中有9个被特异性激活,显然是以非MHC限制的方式,在角质形成细胞或未分离的表皮细胞存在的情况下增殖,这些细胞在体内或体外都用致敏剂处理过。所有7种测试的接触性致敏物质都激活了所有反应性DETC,而用非致敏性刺激物处理的角质形成细胞/表皮细胞与溶剂对照组一样无刺激作用。我们证明DETC与刺激性角质形成细胞/表皮细胞之间需要直接的细胞间接触,且TCR参与了DETC增殖的诱导。DETC对用接触性致敏剂预处理的角质形成细胞或表皮细胞的这种特异性反应性可能表明表皮T细胞参与了接触性敏感性的诱导,并指出了DETC在皮肤免疫系统中的可能作用。

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