首页> 外文期刊>Toxicology Letters: An International Journal Providing a Forum for Original and Pertinent Contributions in Toxicology Research >Photogenotoxicity of hypericin in HaCaT keratinocytes: implications for St. John's Wort supplements and high dose UVA-1 therapy.
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Photogenotoxicity of hypericin in HaCaT keratinocytes: implications for St. John's Wort supplements and high dose UVA-1 therapy.

机译:金丝桃素对HaCaT角质形成细胞的光遗传毒性:对圣约翰草补充剂和高剂量UVA-1治疗的影响。

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摘要

Extract of St. John's Wort (Hypericum perforatum) is commonly used as natural remedy for treatment of mild to moderate depression. However, it contains a powerful photoactive component, hypericin, which can cause a severe photodermatitis when eaten by grazing animals (hypericism). In humans, there is evidence that supplementation with St. John's Wort can reduce the minimal erythemal dose (MED) in patients undergoing high dose UVA-1 phototherapy. This is a recent development in phototherapy where the most erythemogenic parts of the UVA spectrum are filtered out, allowing delivery of higher doses of the longer wavelengths of UVA. Although current published evidence suggests that the plasma levels of hypericin are unlikely to cause clinical phototoxicity, it has been established that photoactive compounds can cause DNA damage at sub-toxic and sub-erythemal doses, the effects of which might not be apparent for many years after the event. The present study used HaCaT keratinocytes to investigate the photoclastogenic ability of hypericin on irradiation with UVA. The results show that although the combination of hypericin and UVA light increased the genotoxic burden, when all factors are taken into account, the risk of significant photogenotoxic damage incurred by the combination of Hypericum extracts and UVA phototherapy may be low in the majority of individuals.
机译:圣约翰草(Hypericum perforatum)的提取物通常用作治疗轻度至中度抑郁症的天然药物。但是,它含有强大的光敏成分金丝桃素,当被放牧的动物食用时会引起严重的光皮炎(催眠症)。在人类中,有证据表明,在接受大剂量UVA-1光疗的患者中,补充圣约翰草可以降低最小红斑剂量(MED)。这是光疗领域的最新进展,其中滤除了UVA光谱的大部分促红细胞生成部分,从而可以提供更高剂量的更长波长的UVA。尽管当前已发表的证据表明血浆金丝桃素水平不太可能引起临床光毒性,但已确定光活性化合物可在亚毒性和亚红剂量下引起DNA损伤,其作用可能多年未见明显在事件发生后。本研究使用HaCaT角质形成细胞来研究金丝桃素对UVA照射的光破细胞能力。结果表明,尽管金丝桃素和UVA光的组合增加了遗传毒性的负担,但考虑到所有因素,金丝桃素提取物和UVA光疗组合引起的显着光遗传毒性损害的风险在大多数个体中可能较低。

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