脂质体包裹的利巴韦林对小鼠裂谷热病毒感染的疗效增强
Enhanced efficacy of liposome-encapsulated ribavirin against Rift Valley fever virus infection in mice.
作者信息
Kende M, Alving C R, Rill W L, Swartz G M, Canonico P G
出版信息
Antimicrob Agents Chemother. 1985 Jun;27(6):903-7. doi: 10.1128/AAC.27.6.903.
Abstract
Administration of liposome-encapsulated ribavirin to mice led to ribavirin concentrations in the liver, the primary site of Rift Valley fever virus proliferation, that were fivefold greater than those attained with the same doses of free ribavirin. Liposomal ribavirin given at a dose of either 25 or 50 mg of drug per kg of body weight protected mice against a rapidly lethal high-titer challenge with Rift Valley fever virus, whereas similar doses of free drug or empty liposomes had no detectable benefit. Hence, tissue targeting of ribavirin with liposomes substantially increased the therapeutic index by increasing the efficacy of the treatment. By using liposomes as drug carriers, a nontoxic, low-dose regimen of ribavirin had a therapeutic effect that was comparable to that achieved with higher but potentially more toxic doses of free ribavirin.
摘要
给小鼠施用脂质体包裹的利巴韦林后,在裂谷热病毒增殖的主要部位肝脏中,利巴韦林的浓度比相同剂量的游离利巴韦林高出五倍。以每千克体重25毫克或50毫克药物的剂量给予脂质体利巴韦林,可保护小鼠免受裂谷热病毒快速致死性高滴度攻击,而相同剂量的游离药物或空脂质体则没有明显效果。因此,脂质体对利巴韦林的组织靶向作用通过提高治疗效果显著提高了治疗指数。通过使用脂质体作为药物载体,无毒、低剂量的利巴韦林治疗方案产生的治疗效果与更高但可能毒性更大的游离利巴韦林剂量相当。
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