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蓝光对正常皮肤的临床和组织学影响。

Clinical and histological effects of blue light on normal skin.

机构信息

Department of Dermatology, Radboud University Nijmegen Medical Centre, Nijmegen, The Netherlands.

出版信息

Photodermatol Photoimmunol Photomed. 2010 Feb;26(1):16-21. doi: 10.1111/j.1600-0781.2009.00474.x.

Abstract

INTRODUCTION

Phototherapy with visible light is gaining interest in dermatological practice. Theoretically, blue light could induce biological effects comparable to ultraviolet A (UVA) radiation.

OBJECTIVES

To study the effects of blue light on normal skin in terms of photodamage, skin ageing and melanogenesis.

METHODS

Eight healthy volunteers were included and irradiation with visible blue light was given on five consecutive days. Skin biopsies were analysed with respect to photodamage (p53, vacuolization, sunburn cells), skin ageing (elastosis, MMP-1) and melanogenesis (Melan-A).

RESULTS

No inflammatory cells and sunburn cells were visible before or after irradiation. A significant increase in the perinuclear vacuolization of keratinocytes was demonstrated during treatment (P=0.02) with a tendency towards significance after cessation of treatment (P=0.09). No significant change in p53 expression was seen. Signs of elastosis and changes in MMP-1 expression were absent. Minimal clinical hyperpigmentation of the irradiated skin was confirmed histologically with a significant increase in Melan-A-positive cells (P=0.03).

CONCLUSIONS

Visible blue light, as given in the present study, does not cause deoxyribonucleic acid damage or early photo-ageing. The biological effects of blue light on normal skin are transient melanogenesis and inexplicable vacuolization without resulting apoptosis. In conclusion, the (short-term) use of visible blue light in dermatological practice is safe.

摘要

简介

可见光疗法在皮肤科实践中越来越受到关注。理论上,蓝光可以产生类似于长波紫外线(UVA)辐射的生物学效应。

目的

研究蓝光对正常皮肤的光损伤、皮肤老化和黑色素生成的影响。

方法

纳入 8 名健康志愿者,连续 5 天进行可见光蓝光照射。用 p53、空泡化、晒伤细胞评估光损伤,用弹性蛋白、MMP-1 评估皮肤老化,用 Melan-A 评估黑色素生成,分析皮肤活检结果。

结果

照射前后均未见炎症细胞和晒伤细胞。治疗期间(P=0.02),可见角质形成细胞核周空泡化明显增加,治疗停止后(P=0.09)有增加趋势。p53 表达无明显变化。未见弹性蛋白迹象和 MMP-1 表达变化。照射皮肤的临床轻度色素沉着通过 Melan-A 阳性细胞的显著增加得到证实(P=0.03)。

结论

本研究中给予的可见光蓝光不会导致脱氧核糖核酸损伤或早期光老化。蓝光对正常皮肤的生物学效应是短暂的黑色素生成和无法解释的空泡化,而不会导致细胞凋亡。总之,在皮肤科实践中短期使用可见光蓝光是安全的。

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