Marutani K, Matsumoto M, Otabe Y, Nagamuta M, Tanaka K, Miyoshi A, Hasegawa T, Nagano H, Matsubara S, Kamide R
Toxicology Research Laboratories, Chugai Pharmaceutical Co. Ltd., Nagano, Japan.
Antimicrob Agents Chemother. 1993 Oct;37(10):2217-23. doi: 10.1128/AAC.37.10.2217.
A newly developed fluoroquinoline, Q-35 (8-OCH3), in which a methoxy group was substituted at the 8 position of the quinoline nucleus, was very stable under irradiation with long-wave UV light (UVA). Derivatives, a fluoroquinolone with no substitution (the 8-H analog) and one in which a fluorine was substituted (the 8-F analog), were degraded in their solutions by the UVA irradiation. The phototoxic inducibility by these derivatives was further studied in a murine model. When mice were dosed orally with 800 mg of Q-35 (8-OCH3) per kg of body weight, the maximum dose given, and exposed to the UVA light, no inflammatory lesions were observed in their ears. Ear redness was marked in mice given more than 12.5 mg of the 8-F analog or 200 mg of the 8-H analog per kg. Histopathological changes, edema, and infiltration of neutrophils were also observed microscopically in groups receiving the 8-H or 8-F analog but not in groups receiving Q-35 (8-OCH3). Similar inflammatory reactions were observed to occur in a dose-dependent manner with other available fluoroquinolone antibacterial agents such as lomefloxacin, enoxacin, norfloxacin, ciprofloxacin and ofloxacin. These results suggest that the introduction of a methoxy group at the 8 position of the quinolone nucleus is important for the reduction of phototoxicity.
一种新开发的氟喹诺酮类药物Q-35(8-甲氧基),其喹啉核的8位被甲氧基取代,在长波紫外线(UVA)照射下非常稳定。其衍生物,即未取代的氟喹诺酮(8-H类似物)和一个氟被取代的衍生物(8-F类似物),在溶液中会被UVA照射降解。在小鼠模型中进一步研究了这些衍生物的光毒性诱导性。当给小鼠按每千克体重口服800毫克Q-35(8-甲氧基)(所给的最大剂量)并暴露于UVA光下时,在它们的耳朵中未观察到炎症损伤。每千克给予超过12.5毫克8-F类似物或200毫克8-H类似物的小鼠耳朵出现明显发红。在接受8-H或8-F类似物的组中,显微镜下也观察到组织病理学变化、水肿和中性粒细胞浸润,但在接受Q-35(8-甲氧基)的组中未观察到。用其他可用的氟喹诺酮类抗菌药物如洛美沙星、依诺沙星、诺氟沙星、环丙沙星和氧氟沙星也观察到类似的炎症反应以剂量依赖性方式发生。这些结果表明在喹诺酮核的8位引入甲氧基对于降低光毒性很重要。
