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体内紫外线A、B和C照射诱导T6-DR+人表皮抗原呈递细胞的剂量反应和时间进程。

Dose response and time course for induction of T6- DR+ human epidermal antigen-presenting cells by in vivo ultraviolet A, B, and C irradiation.

作者信息

Baadsgaard O, Cooper K D, Lisby S, Wulf H C, Wantzin G L

机构信息

Department of Dermatology, Gentofte Hospital, Copenhagen, Denmark.

出版信息

J Am Acad Dermatol. 1987 Nov;17(5 Pt 1):792-800. doi: 10.1016/s0190-9622(87)70265-5.

Abstract

In vivo ultraviolet (UV) exposure of human skin abrogates the antigen-presenting function of T6+ DR+ Langerhans cells and induces the appearance of antigen-presenting T6- DR+ epidermal melanophages. UV-exposed epidermal cells containing T6- DR+ epidermal antigen-presenting cells, in contrast to unexposed epidermal cells containing T6+ DR+ Langerhans cells, potently activate autoreactive regulatory T cells in the absence of exogenous antigens. Autoreactive T cells may be important for regulation of other immune responses such as those which occur in photosensitive lupus erythematosus and in immune surveillance of UV-induced skin cancers. It is therefore imperative to determine the factors that govern their appearance in the skin. It was found that UVB and UVC, but not UVA, induced a dose-dependent appearance of T6- DR+ epidermal melanophages. The optimal time of appearance was 2 or 3 days after UVB and UVC exposure. In contrast, UVA was a poor inducer of T6- DR+ cells at all doses and all time points tested. Although UVA was a poor inducer of T6- DR+ epidermal cells, UVA radiation resulted in depletion of T6+ DR+ Langerhans cells from the epidermis, as did UVB and UVC radiation. This differential effect of UV wave bands on the immunocompetent cells in human skin may be related to the greater potential of UVB exposure to induce skin cancers and to exacerbate systemic lupus erythematosus.

摘要

人体皮肤的体内紫外线(UV)暴露会消除T6⁺DR⁺朗格汉斯细胞的抗原呈递功能,并诱导出现抗原呈递性T6⁻DR⁺表皮黑素巨噬细胞。与含有T6⁺DR⁺朗格汉斯细胞的未暴露表皮细胞相比,含有T6⁻DR⁺表皮抗原呈递细胞的紫外线暴露表皮细胞在无外源性抗原的情况下能有效激活自身反应性调节性T细胞。自身反应性T细胞对于调节其他免疫反应可能很重要,比如在光敏性红斑狼疮以及紫外线诱导的皮肤癌免疫监视中发生的免疫反应。因此,确定控制它们在皮肤中出现的因素至关重要。研究发现,UVB和UVC(而非UVA)会诱导T6⁻DR⁺表皮黑素巨噬细胞呈剂量依赖性出现。出现的最佳时间是UVB和UVC暴露后2或3天。相比之下,在所有测试剂量和所有时间点,UVA都是T6⁻DR⁺细胞的低效诱导剂。尽管UVA是T6⁻DR⁺表皮细胞的低效诱导剂,但UVA辐射会导致表皮中T6⁺DR⁺朗格汉斯细胞减少,UVB和UVC辐射也是如此。紫外线波段对人体皮肤免疫活性细胞的这种差异效应可能与UVB暴露诱导皮肤癌和加重系统性红斑狼疮的更大潜力有关。

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