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一款矿物防晒霜可提供针对紫外线(UV)B和UVA辐射的基因组保护:体外和原位试验。

A mineral sunscreen affords genomic protection against ultraviolet (UV) B and UVA radiation: in vitro and in situ assays.

作者信息

Cayrol C, Sarraute J, Tarroux R, Redoules D, Charveron M, Gall Y

机构信息

Laboratoire de Biologie Cellulaire Cutanée, Institut de Recherche Dermo-Cosmétique Pierre Fabre, Faculté de Médecine Rangueil, 133 route de Narbonne, 31062 Toulouse cedex, France.

出版信息

Br J Dermatol. 1999 Aug;141(2):250-8. doi: 10.1046/j.1365-2133.1999.02973.x.

Abstract

Ultraviolet (UV) radiation has been shown to be responsible for different biological effects on human skin, including the initiation of photocarcinogenesis. Both UVB and UVA have been described as mutagenic, but the processes by which they alter the DNA are different. Although cells can repair DNA damage, some deleterious mutations nevertheless appear and can promote cancer. The risk of photocarcinogenesis is acknowledged and the frequency of photogenodermatosis is increasing. In order to evaluate the protection efficacy of a high sun protection factor (SPF) mineral sunscreen against UVB- and UVA-induced genomic alterations, we have followed two approaches. First, we have tested the sunscreen for its ability to decrease the unscheduled DNA synthesis response in vitro in human fibroblasts, as an indirect measure of UVB-induced lesions (0.005 and 0.01 J/cm2), and second, we have verified its ability to reduce the in situ end-labelling intensity in human skin as a direct measure of UVA-induced single-strand breaks (10 J/cm2). Microscopic analysis clearly demonstrated the protective effect of the sunscreen against UVB and UVA. A dose-dependent effect of mineral sunscreens was observed. There was also a relationship between the SPF and genomic protection. By limiting the accumulation of UV-induced lesions on DNA, this mineral sunscreen could limit the mutation frequency.

摘要

紫外线(UV)辐射已被证明会对人体皮肤产生不同的生物学效应,包括引发光致癌作用。UVB和UVA都被描述为具有致突变性,但它们改变DNA的过程有所不同。尽管细胞能够修复DNA损伤,但仍会出现一些有害突变并可能促进癌症发生。光致癌作用的风险已得到认可,光生性皮肤病的发病率也在上升。为了评估高防晒系数(SPF)的矿物防晒霜对UVB和UVA诱导的基因组改变的防护效果,我们采用了两种方法。首先,我们测试了该防晒霜在体外降低人成纤维细胞中DNA非预定合成反应的能力,以此作为UVB诱导损伤(0.005和0.01 J/cm²)的间接测量方法;其次,我们验证了其降低人体皮肤原位末端标记强度的能力,以此作为UVA诱导单链断裂(10 J/cm²)的直接测量方法。显微镜分析清楚地证明了该防晒霜对UVB和UVA的防护作用。观察到矿物防晒霜具有剂量依赖性效应。防晒系数与基因组保护之间也存在关联。通过限制紫外线诱导的DNA损伤积累,这种矿物防晒霜可以降低突变频率。

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