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首页> 外文期刊>Antiviral chemistry & chemotherapy >Combinations of antiviral and anti-inflammatory preparations for the topical treatment of herpes simplex virus assessed using a murine zosteriform infection model.
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Combinations of antiviral and anti-inflammatory preparations for the topical treatment of herpes simplex virus assessed using a murine zosteriform infection model.

机译:使用鼠类带状疱疹感染模型评估用于局部治疗单纯疱疹病毒的抗病毒和抗炎制剂的组合。

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Recently we have reported a zosteriform murine infection model which employs the adoptive transfer of immune cells (ATI) to recipient infected mice to produce a disease that mimics human recurrent herpes simplex virus (HSV) disease. Mice were infected with HSV-1 by scarification at the lateroventral line of the neck; 2 days later, the mice received immune cells from HSV-1-infected syngeneic mice. Although virus was cleared more quickly from the target tissues of virus replication in recipient mice, ATI resulted in a heightened inflammatory response and delayed healing. This model was used to test the effects of topical formulations containing foscarnet and/or the anti-inflammatory agent, hydrocortisone. Virus clearance and clinical signs, including ear thickness and zosteriform spread of lesions, were studied. Treatment with 3% foscarnet accelerated virus clearance but had little effect on clinical parameters. By contrast, 0.5% hydrocortisone increased the titre and extended the presence of infectious virus for at least 6 days, although the reduction in clinical signs was greater than that obtained with topical foscarnet. Foscarnet in combination with hydrocortisone produced a marked reduction in clinical signs while virus replication was reduced. These results are discussed in relation to the inflammation and discomfort experienced by patients and a possible role for anti-inflammatory formulations in the treatment of HSV reactivation episodes in man.
机译:最近,我们已经报道了一种带状疱疹的小鼠感染模型,该模型采用免疫细胞(ATI)的过继转移到受感染的小鼠身上,产生一种模仿人类复发性单纯疱疹病毒(HSV)疾病的疾病。通过在颈部的后腹侧线划痕使小鼠感染HSV-1。 2天后,小鼠接受了感染HSV-1的同系小鼠的免疫细胞。尽管从受体小鼠的病毒复制目标组织中清除病毒的速度更快,但ATI导致炎症反应增强和愈合延迟。该模型用于测试含有膦甲酸和/或消炎药氢化可的松的局部制剂的作用。研究了病毒清除率和临床体征,包括病灶的耳厚和带状分布。用3%的膦甲酸酯处理可加速病毒清除,但对临床参数影响很小。相比之下,0.5%的氢化可的松可提高滴度并延长传染性病毒的存在至少6天,尽管其临床症状的减轻幅度大于局部使用膦甲酸酯的减轻幅度。膦甲酸与氢化可的松联合使用可显着减少临床症状,同时减少病毒复制。讨论了有关患者经历的炎症和不适以及抗炎制剂在治疗人类HSV活化发作中可能发挥的作用的这些结果。

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