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补骨脂素胺类化合物。3. 5-(氨甲基)-8-甲氧基、5-[[(3-氨丙基)氧基]甲基]和8-[(3-氨丙基)氧基]补骨脂素衍生物的合成、药理行为及与DNA的结合

Psoralenamines. 3. Synthesis, pharmacological behavior, and DNA binding of 5-(aminomethyl)-8-methoxy-, 5-[[(3-aminopropyl)oxy]methyl]-, and 8-[(3-aminopropyl)oxy]psoralen derivatives.

作者信息

Hansen J B, Bjerring P, Buchardt O, Ebbesen P, Kanstrup A, Karup G, Knudsen P H, Nielsen P E, Nordén B, Ygge B

出版信息

J Med Chem. 1985 Aug;28(8):1001-10. doi: 10.1021/jm00146a006.

Abstract

A series of derivatives of 5-(aminomethyl)-8-methoxypsoralens, 8-[(3-aminopropyl)oxy]psoralens, and 5-[[[3-(tri-methylammonio)propyl]methyl]-8-methoxypsoralen has been synthesized and their potential as PUVA reagents examined. While the DNA association constants of selected psoralens were found to be 10(5)-10(6)L mol-1, corresponding to efficient binding, flow linear dichroism studies indicated that only the 8-substituted psoralens bind to DNA by intercalation. Furthermore, the ability to photoinduce interstrand cross-links in calf thymus DNA, in vitro, was as efficient as that of 8-methoxypsoralen for the 8-substituted psoralens, which were up to 25 times as efficient as the 5-substituted psoralens. Four of the psoralens studied were radiolabeled and used to study photobinding to DNA. Analogously to the cross-binding results, the 8-substituted psoralens were more efficiently photobound than the 5-substituted, while only slight differences were found in the photobinding-cross-linking ratio. The photoreactivity of the aminopsoralens toward cyclohexene and 2'-deoxythymidine was enhanced compared to that of 8-methoxypsoralen, the effect being most pronounced when the amino group is close to the furocoumarin ring system. Most of the new compounds were less photocytotoxic than 8-methoxypsoralen to NHIK 3025 cells, in vitro, and they caused less light-induced DNA interstrand cross-linking, in situ, in these cells. A clear correlation between the photocytotoxicity and the DNA cross-linking ability of the psoralens was observed. Several of the derivatives showed more pronounced effects in the light-dependent skin thickening (inflammatory) test on mice than 8-methoxypsoralen. No correlation between DNA cross-linking capacity, in vitro, and skin phototoxicity was found for this series of psoralens.

摘要

已合成了一系列5-(氨甲基)-8-甲氧基补骨脂素、8-[(3-氨丙基)氧基]补骨脂素和5-[[[3-(三甲基铵基)丙基]甲基]-8-甲氧基补骨脂素的衍生物,并研究了它们作为光化学疗法(PUVA)试剂的潜力。虽然选定补骨脂素的DNA结合常数为10⁵ - 10⁶L/mol,表明结合效率较高,但流动线性二色性研究表明,只有8-取代的补骨脂素通过插入作用与DNA结合。此外,在体外,8-取代的补骨脂素在小牛胸腺DNA中光诱导链间交联的能力与8-甲氧基补骨脂素一样高效,其效率比5-取代的补骨脂素高25倍。所研究的四种补骨脂素被放射性标记并用于研究与DNA的光结合。与交联结果类似,8-取代的补骨脂素比5-取代的补骨脂素更有效地进行光结合,而在光结合-交联比率上仅发现微小差异。与8-甲氧基补骨脂素相比,氨基补骨脂素对环己烯和2'-脱氧胸苷的光反应性增强,当氨基靠近呋喃香豆素环系统时,这种效果最为明显。在体外,大多数新化合物对NHIK 3025细胞的光细胞毒性比8-甲氧基补骨脂素小,并且在这些细胞中原位引起的光诱导DNA链间交联也较少。观察到补骨脂素的光细胞毒性与DNA交联能力之间存在明显的相关性。几种衍生物在对小鼠的光依赖性皮肤增厚(炎症)试验中比8-甲氧基补骨脂素表现出更明显的效果。对于这一系列补骨脂素,未发现体外DNA交联能力与皮肤光毒性之间存在相关性。

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