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[光疗与致癌作用]

[Phototherapy and carcinogenesis].

作者信息

Hofbauer G

机构信息

Dermatologische Klinik, Universitätsspital Zürich, Gloriastr. 31, 8091 Zürich, Schweiz.

出版信息

Hautarzt. 2013 May;64(5):349-53. doi: 10.1007/s00105-013-2587-0.

Abstract

Phototherapy successfully uses the short-term effects of ultraviolet light against inflammation and proliferation. For its long-term effects, however, ultraviolet light was recently classified as a carcinogen. The wave spectrum employed in phototherapy has various carcinogenic effects in experimental systems, most notably DNA mutations in keratinocytes. Clinically, PUVA increases the risk for squamous cell carcinoma of the skin, especially after following 350 or more phototherapy sessions over a lifetime. Melanoma and genital skin cancer are not increased by PUVA alone. Previous UV damage, immunosuppression and other systemic treatments increase cutaneous carcinogenesis through PUVA. In contrast, broad-band UVB, narrow-band UVB and UVA1 have not yet been linked to cutaneous carcinogenesis, but will need careful follow-up in larger studies. Phototherapy remains a safe treatment modality, provided that the indication is well-founded, previous exposure and co-carcinogens are considered, and short and dose-intensive treatment protocols are favored, PUVA is chosen as second-line treatment that should not be used for more than a lifetime total of 250-300 phototherapy sessions.

摘要

光疗成功利用了紫外线对炎症和增殖的短期效应。然而,就其长期效应而言,紫外线最近被归类为致癌物。光疗中使用的光谱在实验系统中具有多种致癌作用,最显著的是角质形成细胞中的DNA突变。临床上,补骨脂素加紫外线A疗法(PUVA)会增加皮肤鳞状细胞癌的风险,尤其是在一生中接受350次或更多次光疗后。单独使用PUVA不会增加黑色素瘤和生殖器皮肤癌的发病率。先前的紫外线损伤、免疫抑制和其他全身治疗会通过PUVA增加皮肤致癌作用。相比之下,宽带中波紫外线(UVB)、窄带UVB和长波紫外线1(UVA1)尚未与皮肤致癌作用相关联,但在更大规模的研究中需要仔细随访。只要适应症合理、考虑到先前的暴露情况和协同致癌物,并且倾向于采用短期和高剂量的治疗方案,光疗仍然是一种安全的治疗方式,PUVA应作为二线治疗选择,一生中使用次数不应超过250 - 300次光疗。

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