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Cutaneous infections of mice with vaccinia or cowpox viruses and efficacy of cidofovir.

机译:牛痘或牛痘病毒小鼠的皮肤感染和西多福韦的功效。

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摘要

Orthopoxviruses, including smallpox, monkeypox and molluscipox, pose risks to human health through bioterrorist acts or natural transmission. There is no approved therapy for orthopoxvirus infections; however, cidofovir (CDV) has been approved as an investigational new drug for emergency treatment of adverse effects following smallpox vaccination. For evaluation of new therapies directed against orthopoxvirus infections, we have utilized immunocompetent, hairless mice (SKH-1) inoculated by a cutaneous route with cowpox virus (CV) or vaccinia virus (VV). Mice subsequently developed skin lesions and virus was recovered from the site of inoculation and quantified. Skin biopsies were evaluated microscopically, revealing brick-like eosinophilic, intracytoplasmic inclusion bodies characteristic of orthopoxvirus infection. SKH-1 mice fully recovered from either CV or VV infection. Immunodeficient Athymic or Rhino mice inoculated with CV or VV had more lesions and severe disease than SKH-1 mice. CV-infected SKH-1 mice were treated either with systemic or topical CDV. Although some protection was achieved with systemic treatment, 5% topical CDV was most effective at reducing virus titers in skin, lung, kidney, and spleen. These models may provide a means for evaluating efficacy of new therapies directed against orthopoxvirus diseases and further confirm the topical activity of CDV against cutaneous infections.
机译:正痘病毒,包括天花,猴痘和软体动物,通过生物恐怖行为或自然传播对人类健康构成威胁。没有批准的正痘病毒感染疗法。但是,西多福韦(CDV)已被批准作为研究性新药用于紧急治疗天花疫苗接种后的不良反应。为了评估针对正痘病毒感染的新疗法,我们利用了具有免疫能力的无毛小鼠(SKH-1),该小鼠通过皮肤途径接种了牛痘病毒(CV)或牛痘病毒(VV)。小鼠随后出现皮肤损伤,并从接种部位回收病毒并定量。显微镜检查皮肤活组织检查,发现正痘病毒感染特征性的砖样嗜酸性,胞浆内包涵体。 SKH-1小鼠可从CV或VV感染中完全康复。与SKH-1小鼠相比,接种CV或VV的免疫缺陷性无胸腺或犀牛小鼠具有更多的病变和严重的疾病。用全身或局部CDV治疗感染CV的SKH-1小鼠。尽管通过全身治疗获得了一定程度的保护,但是5%的局部CDV在减少皮肤,肺,肾脏和脾脏中的病毒效价方面最有效。这些模型可以为评估针对正痘病毒疾病的新疗法的疗效提供一种手段,并进一步证实CDV对皮肤感染的局部活性。

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