单功能和双功能呋喃香豆素的致癌作用。

National Cancer Institute monograph Pub Date : 1984-12-01
M P Mullen, M A Pathak, J D West, T J Harrist, F Dall'Acqua
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引用次数: 0

摘要

我们启动了这些研究,以确定双功能(链间交联)补骨脂素,如8-甲氧基补骨脂素(8-MOP)是否比单功能补骨脂素(如angelicin或异补骨脂素衍生物)和3-碳氧基孢子素(3-CP)更具致癌性。无毛小鼠(Skh:hr-1)每组40只,每周治疗3次,持续12 ~ 15个月。共17组,研究5种补骨脂素[8-MOP、3-CP、5-甲基当归素、4,5′-二甲基当归素(4,5′-DMA)、当归素]的光致癌作用。在暴露于UVA (320-400 nm)辐射(0.1、2.5或7.5焦耳/cm2)前45分钟,将0.01-0.1%补骨脂素乙醇溶液以5.0或50微克/cm2的剂量从颈椎到腰椎局部涂抹。对照组只接受药物应用或UVA暴露。研究表明,异补骨脂素,如5-甲基angelicin或4,5'-DMA,形成单功能加合物比双功能补骨脂素更致癌。达到50%肿瘤发生率所需的潜伏期和时间,8-MOP比4,5'-DMA或5-甲基angelicin要长得多。用后两种化合物处理的小鼠比用8-MOP处理的小鼠肿瘤数量更多,体积更大。单功能的当归素是弱致癌性的,而3-CP,也是单功能的补骨脂素,是非致癌性的。组织学检查显示8-MOP、5-甲基angelicin、4,5′-DMA诱导的肿瘤均为鳞状细胞癌。由于其皮肤光敏特性和诱导链间交联的能力以及在复制过程中对DNA的严重损伤,双功能补骨脂素显然比单功能异补骨脂素对细胞产生更致命的损伤。(摘要删节250字)
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Carcinogenic effects of monofunctional and bifunctional furocoumarins.

We initiated these studies to determine whether bifunctional (interstrand cross-linking) psoralens, such as 8-methoxypsoralen (8-MOP), are more carcinogenic than are the monofunctional, such as angelicin or isopsoralen derivatives, and 3-carbethoxysporalen (3-CP). Hairless mice (Skh:hr-1) in groups of 40 were treated three times weekly for 12 to 15 months. There were 17 groups, and the photocarcinogenic effects of 5 psoralens [8-MOP, 3-CP, 5-methylangelicin, 4,5'-dimethylangelicin (4,5'-DMA), and angelicin] were investigated. Ethanolic solutions of 0.01-0.1% psoralens were topically applied at 5.0 or 50 micrograms/cm2 from cervical to lumbar regions 45 minutes before exposure to UVA (320-400 nm) radiation (0.1, 2.5, or 7.5 joules/cm2). Control groups received either the drug application or UVA exposure only. The study revealed that isopsoralens, such as 5-methylangelicin or 4,5'-DMA, that form monofunctional adducts are more carcinogenic than bifunctional psoralens. The latency and time required for 50% prevelance of tumors was much longer with 8-MOP than with 4,5'-DMA or 5-methylangelicin. Mice treated with the latter 2 compounds had a greater number and larger tumors than mice treated with 8-MOP. The monofunctional angelicin was weakly carcinogenic, whereas 3-CP, also a monofunctional psoralen, was noncarcinogenic. Histologic examination revealed that tumors induced by 8-MOP, 5-methylangelicin, or 4,5'-DMA were all squamous cell carcinomas. Because of their skin-photosensitizing property and their ability to induce interstrand cross-links and severe damage to DNA in replication, bifunctional psoralens apparently produce more lethal damage in cells than do monofunctional isopsoralens.(ABSTRACT TRUNCATED AT 250 WORDS)

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