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UVB photolysis of hydrocortisone 21-acetate.

机译:氢化可的松21-乙酸酯的UVB光解。

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摘要

Hydrocortisone 21-acetate (HCA) in methanol solution undergoes photodegradation under UVB light, as monitored by HPLC. Five main photoproducts have been isolated and characterized by means of NMR and mass spectroscopy. One of them derives from a Norrish I photoreaction which cleaves the C17-C20 bond of the steroid yielding the andro-derivative, a second product comes from a Yang-type photorearrangement which links C18 to C20 yielding a cyclobutane adduct. The former photoproduct, in turn, undergoes further photolysis giving rise to various photoproducts, of which three have been characterized. The first is a stereoisomer of the andro-derivative, the others arise from the opening of the five-membered ring. HCA also proved photounstable in the solid state and in a commercial formulation for topical use, thus confirming the requirements of the Pharmacopeias for light protection of this drug. Indeed, experiments on LPS-stimulated THP-1 cells demonstrated the loss of anti-inflammatory activity when HCA was UVB-photodegraded. The radical mechanism involved in HCA photolysis seems also responsible for the in vitro photohemolytic effect and lipid peroxidation induced by HCA in combination with UVB light.
机译:用HPLC监测,甲醇溶液中的21-醋酸氢化可的松(HCA)在UVB光下发生光降解。已分离出五种主要的光产物,并通过NMR和质谱进行了表征。其中之一来自于Norrish I光反应,该反应裂解了类固醇的C17-C20键,生成了雄激素衍生物,第二个产品来自于将C18连接至C20的杨型光重排,从而生成了环丁烷加合物。继而,前一种光产物经历进一步的光解,产生了各种光产物,其中三种已被表征。第一个是雄激素衍生物的立体异构体,其他是五元环的开环。 HCA还被证明在固态和用于局部使用的商业制剂中是光不稳定的,因此证实了药典对这种药物的光保护的要求。实际上,在LPS刺激的THP-1细胞上进行的实验表明,当HCA被UVB光降解时,抗炎活性会丧失。参与HCA光解的自由基机制似乎也与HCA结合UVB光诱导的体外光溶血作用和脂质过氧化作用有关。

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