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首页> 外文期刊>Photochemistry and Photobiology: An International Journal >On the photobiological properties of chimeras combining quaternary ammonium derivatives of retinoic amides and psoralen. A study with cultured human keratinocytes
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On the photobiological properties of chimeras combining quaternary ammonium derivatives of retinoic amides and psoralen. A study with cultured human keratinocytes

机译:视黄酰胺和补骨脂素的季铵衍生物结合的嵌合体的光生物学特性。培养的人类角质形成细胞的研究

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摘要

The effectiveness of the combination of retinoids with 8-methoxypsoralen (8-MOP) and ultraviolet-A (UV-A) light in the treatment of some cutaneous proliferative diseases has motivated the synthesis of new "chimera-type" molecules built from psoralen derivatives and retinoic amides and related molecules. The chimeras result from the combination of 8-(3-bromopropyloxy)-psoralen with amides prepared by reacting 4-amino-pyridine with 13E- and 13Z-retinoic acids or a "retinoid-like" derivative with an alkene chain of only three double bonds. The synthesis of chimeras built with the 8-(3-bromopropyloxy)-psoralen and the amide of cinnamic acid or its 4-methoxy derivative has also been carried out. In contrast to 8-MOP, all the chimeras exhibit strong molar absorptivities in the range 20 000-40 000 M-1 cm(-1) in the 340-390 ran UV-A region. The "retinoid-like"- and retinoid-psoralen chimeras are characterized by a marked dark toxicity toward proliferating NCTC 2544 keratinocytes (with a lethal dose corresponding to 50% cell survival [LD50] of 1-5 muM) as compared with that of the cinnamic acid derivative-psoralen chimeras (LD50 greater than or equal to 50 muM). This toxicity leads to alteration of the mitochondrial membrane potential. At nontoxic concentrations, the chimeras demonstrate effective psoralens + UV-A-induced photocytotoxicity. They are moderate photo-sensitizers of membrane lipid peroxidation. Cell apoptosis is a major photocytotoxic process as suggested by the fluorescence-activated cell-sorting technique using annexin-fluorescein isothiocyanate and propidium iodide as apoptotic markers. [References: 35]
机译:类视黄醇与8-甲氧基补骨脂素(8-MOP)和紫外线-A(UV-A)光的组合在治疗某些皮肤增生性疾病中的有效性促进了由补骨脂素衍生物构建的新“嵌合体型”分子的合成以及视黄酰胺和相关分子。嵌合体是由8-(3-溴丙氧基)-补骨脂素与酰胺结合而成的,酰胺是通过使4-氨基吡啶与13E-和13Z-视黄酸或“类视黄醇”衍生物与只有三个双链烯烃的链反应而制得的债券。还已经合成了由8-(3-溴丙氧基)-补骨脂素和肉桂酸的酰胺或其4-甲氧基衍生物构成的嵌合体。与8-MOP相比,所有嵌合体在340-390 nm的UV-A区域中显示出在20 000-40 000 M-1 cm(-1)范围内的强摩尔吸收率。 “类视黄醇”-和类视黄醇-补骨脂素嵌合体的特征是与增殖的NCTC 2544角质形成细胞(致死剂量相当于1-5μM的50%细胞存活率[LD50])具有显着的暗毒性。肉桂酸衍生物-补骨脂素嵌合体(LD50大于或等于50μM)。这种毒性导致线粒体膜电位的改变。在无毒浓度下,嵌合体表现出有效的补骨脂素+ UV-A诱导的光细胞毒性。它们是膜脂质过氧化的中度光敏剂。如使用膜联蛋白-异硫氰酸荧光素和碘化丙啶作为凋亡标记的荧光激活细胞分选技术所暗示的,细胞凋亡是主要的光细胞毒性过程。 [参考:35]

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