Local effects of UV radiation on immunization with contact sensitizers. I. Down-regulation of contact hypersensitivity by application of TNCB to UV-irradiated skin.

Photo-dermatology Pub Date : 1988-06-01
P D Cruz, J Nixon-Fulton, R E Tigelaar, P R Bergstresser
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Abstract

Exposure of mouse skin to UV radiation in doses comparable to those commonly received by humans has been shown to diminish the capacity of irradiated skin to mediate the induction of contact hypersensitivity to dinitrofluorobenzene (DNFB). In other studies, contact sensitization reactions to the structurally related hapten, trinitrochlorobenzene (TNCB), have been used to test the immunogenic properties of haptenated subpopulations of epidermal cells. To extend the applicability of TNCB to experiments that examine UVB modulation of immunization by epidermal cells, we examined the sensitivity of TNCB-induced contact hypersensitivity to low doses of UVB radiation. Abdominal skin of C3H mice was exposed to daily doses of 660 J/m2 broad-band UV radiation for 4 successive days. Immediately following the final exposure, 7% TNCB was applied to irradiated or non-irradiated skin of designated mice. After 5 days, mice were ear-challenged with 2% TNCB, and incremental ear-swelling responses were measured. Mice sensitized with TNCB through irradiated skin exhibited significantly diminished responses compared with UVB-treated mice sensitized through non-irradiated skin. We also found that mice initially sensitized with TNCB through irradiated skin but subsequently painted with oxazolone on normal skin developed full responses to ear-challenge with oxazolone. In contrast, mice sensitized initially with TNCB through irradiated skin failed to fully immunize even after TNCB was repainted on normal skin at a later date. We conclude that low-dose UVB radiation interrupts the induction of contact hypersensitivity to TNCB, leading to hapten-specific nonresponsiveness rather than hypersensitivity, and that this capacity to prevent successful immunization with TNCB is limited to the site of irradiation.(ABSTRACT TRUNCATED AT 250 WORDS)

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紫外线辐射对接触致敏剂免疫的局部影响。1 .紫外光照射皮肤应用TNCB下调接触性超敏反应。
将小鼠皮肤暴露在与人类通常接受的剂量相当的紫外线辐射下,已证明会降低受照射皮肤介导对二硝基氟苯(DNFB)接触性超敏反应的能力。在其他研究中,对结构相关的半抗原三硝基氯苯(TNCB)的接触致敏反应已被用于测试表皮细胞半抗原亚群的免疫原性。为了将TNCB的适用性扩展到检测中波辐射对表皮细胞免疫调节的实验中,我们检测了TNCB诱导的接触超敏反应对低剂量中波辐射的敏感性。将C3H小鼠腹部皮肤连续4天暴露于660 J/m2的宽带紫外线辐射下。在最后一次暴露后,将7% TNCB立即应用于指定小鼠的辐照或未辐照皮肤。5天后,用2%的TNCB刺激小鼠耳,并测量耳肿胀反应。与未照射皮肤致敏的uvb处理小鼠相比,通过照射皮肤致敏的TNCB小鼠的反应明显减弱。我们还发现,最初通过辐照皮肤致敏TNCB的小鼠,随后在正常皮肤上涂上恶唑酮,对恶唑酮的耳朵攻击产生完全反应。相比之下,最初通过辐照皮肤致敏的小鼠即使在稍后将TNCB重新涂在正常皮肤上也未能完全免疫。我们得出结论,低剂量UVB辐射阻断了对TNCB接触性超敏反应的诱导,导致半抗原特异性无反应而不是超敏反应,并且这种阻止TNCB成功免疫的能力仅限于照射部位。(摘要删节250字)
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