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首页> 外文期刊>Mutation Research: International Journal on Mutagenesis, Chromosome Breakage and Related Subjects >Sunless skin tanning with dihydroxyacetone delays broad-spectrum ultraviolet photocarcinogenesis in hairless mice.
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Sunless skin tanning with dihydroxyacetone delays broad-spectrum ultraviolet photocarcinogenesis in hairless mice.

机译:用二羟基丙酮晒日光浴的皮肤会延迟无毛小鼠的广谱紫外线光致癌作用。

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摘要

Sunless tanning with dihydroxyacetone (DHA) is not considered to be a sunscreen although it does absorb parts of the ultraviolet (UV) spectrum. We investigated the protection with topical application of DHA against solar UV-induced skin carcinogenesis in lightly pigmented hairless hr/hr C3H/Tif mice. Broad-spectrum UV radiation, simulating the UV part of the solar spectrum was obtained from one Philips TL12 and five Bellarium-S SA-1-12 tubes. Three groups of mice were UV-exposed four times a week to a dose-equivalent of four times the standard erythema dose (SED), without or with application of 5 or 20% DHA only twice a week. Similarly, three groups of mice were treated with DHA and irradiated with a high UV dose (8 SED), simulating a skin burn. Two groups (controls) were not irradiated, but either left untreated or treated with 20% DHA alone. The UV-induced skin pigmentation by melanogenesis could easily be distinguished from DHA-induced browning and was measured by a non-invasive, semi-quantitative method. Application of 20% DHA reduced by 63% the pigmentation produced by 4 SED, however, only by 28% the pigmentation produced by 8 SED. Furthermore, topical application of 20% DHA significantly delayed the time to appearance of the first tumor >/=1mm (P=0.0012) and the time to appearance of the third tumor (P=2x10(-6)) in mice irradiated with 4 SED. However, 20% DHA did not delay tumor development in mice irradiated with 8 SED. Application of 5% DHA did not influence pigmentation or photocarcinogenesis.In conclusion, this is the first study to show that the superficial skin coloring generated by frequent topical application of DHA in high concentrations may delay skin cancer development in hairless mice irradiated with moderate UV doses.
机译:尽管二羟基丙酮(DHA)确实吸收了部分紫外线(UV)光谱,但它不被认为是防晒霜。我们调查了局部应用DHA对浅色无毛hr / hr C3H / Tif小鼠中太阳紫外线引起的皮肤癌发生的保护作用。从一根飞利浦TL12和五个Bellarium-S SA-1-12管获得了模拟太阳光谱中紫外线部分的广谱UV辐射。三组小鼠每周进行四次紫外线照射,剂量相当于标准红斑剂量(SED)的四倍,每周不使用或仅使用5%或20%DHA进行两次。同样,三组小鼠用DHA治疗并用高紫外线剂量(8 SED)照射,模拟皮肤灼伤。两组(对照组)未接受辐照,但未经治疗或仅接受20%DHA治疗。紫外线引起的黑色素引起的皮肤色素沉着很容易与DHA引起的褐变区分开,并通过非侵入性,半定量方法进行测量。施用20%DHA可使4 SED产生的色素沉着减少63%,但是,仅使8 SED产生的色素沉着减少28%。此外,局部照射20%DHA显着延迟了用4辐照的小鼠出现第一个肿瘤的时间> / = 1mm(P = 0.0012)和出现第三个肿瘤的时间(P = 2x10(-6))。 SED。但是,用8 SED辐照的小鼠中20%的DHA不会延迟肿瘤的发展。 5%DHA的使用不会影响色素沉着或光致癌作用。总而言之,这是第一项研究,表明频繁以高浓度DHA局部局部应用所产生的浅层皮肤着色可能会延迟用中度紫外线剂量照射的无毛小鼠的皮肤癌发展。

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