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紫外线A1(340 - 400纳米)照射与系统性红斑狼疮

Ultraviolet A1 (340-400 nm) irradiation and systemic lupus erythematosus.

作者信息

McGrath H

机构信息

Department of Medicine, Louisiana State University, New Orleans, USA.

出版信息

J Investig Dermatol Symp Proc. 1999 Sep;4(1):79-84. doi: 10.1038/sj.jidsp.5640187.

Abstract

Short wavelengths of ultraviolet (UV) light are clearly harmful in systemic lupus erythematosus (SLE), but the action of long UV wavelengths in SLE is more enigmatic. In a series of animal and human studies, long-wavelength UV radiation, i.e., radiation in the ultraviolet-A1 (UVA1) range (340-400 nm), has proven effective in the treatment of SLE. Disease amelioration and a marked decrease in mortality followed ultraviolet-A (UVA) radiation (320-400 nm) of the New Zealand White/New Zealand Black mouse model of lupus. A follow-up study in the same animal suggested that the longer wavelengths (UVA1, 340-400 nm) in the UVA wave band were primarily responsible. There followed four human studies. The first three of these provided data indicating that low-dose UVA1 radiation significantly reduced constitutional symptoms, joint pain, rashes, and the systemic lupus activity measures, a validated gauge of disease activity in SLE. The fourth human study showed that the therapeutic action of low-dose UVA1 action persisted or progressed long term, a period averaging 3.4 y. UVA1 effects on DNA repair, cell-mediated immunosuppression, tumor necrosis factor alpha release, and apoptosis contrast markedly with those of ultraviolet B (UVB, 280-320 nm) radiation and afford a possible basis for the salutary action of this modality of treatment. The unique features of UVA1 wavelengths may be suited to further therapeutic use, not only in SLE but also in other immunologic disorders.

摘要

短波长紫外线(UV)对系统性红斑狼疮(SLE)显然有害,但长波长紫外线在SLE中的作用更具神秘性。在一系列动物和人体研究中,长波长紫外线辐射,即紫外线A1(UVA1)范围内(340 - 400纳米)的辐射,已被证明对SLE治疗有效。对新西兰白兔/新西兰黑鼠狼疮模型进行紫外线A(UVA,320 - 400纳米)辐射后,疾病得到改善,死亡率显著降低。对同一动物的后续研究表明,UVA波段中较长波长(UVA1,340 - 400纳米)起主要作用。随后有四项人体研究。其中前三项研究提供的数据表明,低剂量UVA1辐射能显著减轻全身症状、关节疼痛、皮疹以及系统性红斑狼疮活动指标,这是一种经过验证的SLE疾病活动衡量标准。第四项人体研究表明,低剂量UVA1的治疗作用长期持续或进展,平均为期3.4年。UVA1对DNA修复、细胞介导的免疫抑制、肿瘤坏死因子α释放和细胞凋亡的影响与紫外线B(UVB,280 - 320纳米)辐射的影响明显不同,为这种治疗方式的有益作用提供了可能的依据。UVA1波长的独特特性可能适合进一步用于治疗,不仅适用于SLE,也适用于其他免疫性疾病。

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