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烯丙基氢过氧化物的合成及铁体系中自由基形成的 EPR 自旋捕获研究——作为增敏途径引发剂的潜在自由基。

Synthesis of allylic hydroperoxides and EPR spin-trapping studies on the formation of radicals in iron systems as potential initiators of the sensitizing pathway.

机构信息

Laboratoire de Dermatochimie, Institut de Chimie de Strasbourg (UMR 7177), Université de Strasbourg, 4 Rue Blaise Pascal, 67081 Strasbourg, France.

出版信息

J Org Chem. 2011 Aug 5;76(15):6188-200. doi: 10.1021/jo200948x. Epub 2011 Jun 28.

DOI:10.1021/jo200948x
PMID:21648947
Abstract

Many terpenes used as fragrance compounds autoxidize when exposed to air, forming allylic hydroperoxides that have the potential to be skin contact allergens. To trigger the immunotoxicity process that characterizes contact allergy, these hydroperoxides are supposed to bind covalently to proteins in the skin via radical pathways. We investigated the formation of reactive radical intermediates from 7-hydroperoxy-3,7-dimethylocta-1,5-dien-3-ol and 2-hydroperoxylimonene, responsible for the sensitizing potential acquired by autoxidized linalool and limonene. Both compounds were synthesized through new short and reproducible synthetic pathways. The hydroperoxide decomposition catalyzed by Fe(II)/Fe(III) redox systems, playing a key role in degradating peroxides in vivo, was examined by spin-trapping-EPR spectroscopy. Alkoxyl and carbon-centered free radicals derived from the hydroperoxides were successfully trapped by the spin-trap 5,5-dimethyl-1-pyrroline N-oxide, whereas peroxyl radicals were characterized by spin-trapping studies with 5-diethoxyphosphoryl-5-methyl-1-pyrroline N-oxide. Using liquid chromatography combined with mass spectrometry, we demonstrated the formation of adducts, via radical mechanisms induced by Fe(II)/Fe(III), between the hydroperoxides and N-acetylhistidine methyl ester, a model amino acid that is prone to radical reactions. Free radicals derived from these hydroperoxides can thus induce amino acid chemical modifications via radical mechanisms. The study of these mechanisms will help to understand the sensitizing potential of hydroperoxides.

摘要

许多萜烯类化合物在暴露于空气中时会自动氧化,形成具有潜在皮肤接触过敏原的烯丙基过氧化物。为了引发接触过敏所特有的免疫毒性过程,这些过氧化物应该通过自由基途径与皮肤中的蛋白质共价结合。我们研究了 7-过氧-3,7-二甲基辛-1,5-二烯-3-醇和 2-过氧柠檬烯形成的反应性自由基中间体,这两种化合物负责使自动氧化的芳樟醇和柠檬烯获得致敏潜能。这两种化合物都是通过新的短而可重复的合成途径合成的。Fe(II)/Fe(III)氧化还原体系催化的过氧化物分解在体内降解过氧化物中起着关键作用,通过自旋捕获 EPR 光谱进行了研究。过氧化物衍生的烷氧基和碳中心自由基通过自旋捕获 5,5-二甲基-1-吡咯啉 N-氧化物成功捕获,而过氧自由基通过自旋捕获研究用 5-二乙氧基膦酰基-5-甲基-1-吡咯啉 N-氧化物进行了表征。使用液相色谱与质谱联用,我们证明了在 Fe(II)/Fe(III)诱导的自由基机制下,过氧化物与 N-乙酰组氨酸甲酯(一种容易发生自由基反应的模型氨基酸)之间形成了加合物。因此,这些过氧化物衍生的自由基可以通过自由基机制诱导氨基酸的化学修饰。这些机制的研究将有助于理解过氧化物的致敏潜能。

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