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Evaluation of imiquimod for topical treatment of vaccinia virus cutaneous infections in immunosuppressed hairless mice.

机译:咪喹莫特用于免疫抑制的无毛小鼠局部治疗牛痘病毒皮肤感染的评估。

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Imiquimod is an immune response modifier prescribed as a topical medication for a number of viral and neoplastic conditions. We evaluated the antiviral activity of imiquimod against vaccinia virus (WR strain) cutaneous infections in immunosuppressed (with cyclophosphamide) hairless mice when administered after virus exposure. Primary lesions progressed in severity, satellite lesions developed, and infection eventually killed the mice. Once daily topical treatment with 1% imiquimod cream for 3, 4, or 5 days were compared to twice daily topical treatment with 1% cidofovir cream for 7 days. Survival time of mice in all treated groups was significantly prolonged compared to placebo controls. The mean day of death for the placebo group, 3-day imiquimod, 4-day imiquimod, 5-day imiquimod, and cidofovir groups were 15.5, 20.0, 20.5, 19.5, and 20.5 days post-infection, respectively. All treatment groups showed significant reductions in primary lesion size and in the number of satellite lesions. The cidofovir and 4-day imiquimod treatments delayed the appearance of lung virus titers by 3 and 6 days, respectively, although cutaneous lesion and snout virus titers were not as affected by treatment. Benefits in survival and lesion reduction were observed when imiquimod treatment was delayed from 24, 48, and 72 h post-infection. However, increasing the treatment dose of imiquimod from 1% to 5% led to a significant decrease in antiviral efficacy. These results demonstrate the protective effects of topically administered imiquimod against a disseminated vaccinia virus infection in this mouse model.
机译:咪喹莫特(Imiquimod)是一种免疫应答调节剂,被指定为多种病毒和肿瘤疾病的局部用药。我们评估了咪喹莫特对暴露于免疫抑制(使用环磷酰胺)的无毛小鼠中的牛痘病毒(WR株)皮肤感染的抗病毒活性。原发性病变的严重程度不断提高,卫星病变逐渐发展,感染最终杀死了小鼠。将每天一次用1%咪喹莫特乳膏进行3、4或5天的局部治疗与每天两次用1%西多福韦乳膏进行7天的局部治疗进行比较。与安慰剂对照相比,所有治疗组中小鼠的存活时间均显着延长。安慰剂组,3天咪喹莫特,4天咪喹莫特,5天咪喹莫特和西多福韦组的平均死亡天数分别为感染后15.5、20.0、20.5、19.5和20.5天。所有治疗组均显示原发灶大小和附属病变数目显着减少。西多福韦和咪喹莫特4天治疗分别使肺病毒滴度的出现延迟了3天和6天,尽管皮肤病变和鼻部病毒滴度不受治疗的影响。当将咪喹莫特治疗从感染后24、48和72小时延迟时,观察到了对存活和减少病变的益处。但是,将咪喹莫特的治疗剂量从1%增加到5%会导致抗病毒功效显着下降。这些结果证明了在该小鼠模型中局部施用的咪喹莫特对弥散的牛痘病毒感染的保护作用。

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