Dunnick J K, Forbes P D, Davies R E, Iverson W O
Toxicol Appl Pharmacol. 1987 Jun 15;89(1):73-80. doi: 10.1016/0041-008x(87)90177-3.
An experimental design to simulate PUVA therapy (oral 8-methoxypsoralen followed by uv radiation) has been tested in a 13-week subchronic study to determine the relative toxicities of 8-methoxypsoralen (8-MOP), 5-methoxypsoralen (5-MOP), 5-methylisopsoralen (5-MIP), and 3-carbethoxypsoralen (3-CEP) in inbred hairless mice (HRA/Skh). Drug was administered by 1-hr pulse feedings three times a week after mice were fasted overnight; individually housed animals were then exposed to uv radiation (320-400 nm; less than 2% output less than 320 nm). 8-MOP or 5-MOP administered orally (at doses of approximately 240 or 480 mg/m2 body surface area per week) followed one-half hour later with uv radiation of 2 J/cm2 for 13 weeks were found to cause skin toxicity including inflammation, hyperplasia, ulceration, and cellular atypia. Dose-related toxicity was not seen in other organ systems. Corresponding levels of 5-MIP or 3-CEP with uv radiation did not produce skin toxicity. These studies show that the psoralens with two potential DNA-binding sites (8-MOP and 5-MOP) were more toxic than psoralens with only one photoreactive site (5-MIP and 3-CEP).
一种模拟补骨脂素紫外线A光疗法(口服8-甲氧基补骨脂素后进行紫外线辐射)的实验设计,已在一项为期13周的亚慢性研究中进行测试,以确定8-甲氧基补骨脂素(8-MOP)、5-甲氧基补骨脂素(5-MOP)、5-甲基异补骨脂素(5-MIP)和3-乙氧羰基补骨脂素(3-CEP)在近交系无毛小鼠(HRA/Skh)中的相对毒性。在小鼠过夜禁食后,每周通过1小时的脉冲喂食给药3次;然后将单独饲养的动物暴露于紫外线辐射(320 - 400纳米;小于320纳米的输出小于2%)。口服8-MOP或5-MOP(每周剂量约为240或480毫克/平方米体表面积),半小时后进行2焦耳/平方厘米的紫外线辐射,持续13周,结果发现会导致皮肤毒性,包括炎症、增生、溃疡和细胞异型性。在其他器官系统中未观察到剂量相关的毒性。5-MIP或3-CEP与紫外线辐射的相应水平未产生皮肤毒性。这些研究表明,具有两个潜在DNA结合位点的补骨脂素(8-MOP和5-MOP)比仅具有一个光反应位点的补骨脂素(5-MIP和3-CEP)毒性更大。
