首页> 外文期刊>Archives of virology >The efficacy of a DNA vaccine encoding herpes simplex virus type 1 (HSV-1) glycoprotein D in decreasing ocular disease severity following corneal HSV-1 challenge.
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The efficacy of a DNA vaccine encoding herpes simplex virus type 1 (HSV-1) glycoprotein D in decreasing ocular disease severity following corneal HSV-1 challenge.

机译:编码1型单纯疱疹病毒(HSV-1)糖蛋白D的DNA疫苗在降低角膜HSV-1攻击后降低眼部疾病严重程度方面的功效。

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摘要

Antiviral effects of a DNA vaccine against herpes simplex virus 1 (HSV-1) glycoprotein D (gD) were evaluated in eight week-old female BALB/c mice. The nuclease-insensitive construct (gD-ASOR) consisted of an HSV-1 gD encoding plasmid coupled to asialo orosomucoid (ASOR), targeting it to cells bearing ASOR receptors. Mice were immunized on day 0 and 7 with 10 microg doses of gD-ASOR or control substances. Fourteen days later, mice were infected by the corneal route with 10(5) pfu or 10(6) pfu HSV-1, strain 17syn+. Immunized mice showed a significant decrease in ocular disease severity over a 21-day observation period following infection compared to sham-immunized mice. Acute replication kinetic assays demonstrated a 100-fold decrease in viral titers on day 6 in trigeminal ganglia from immunized BALB/c mice compared to sham-immunized mice. Immunized mice showed a significant increase in numbers of CD4(+)T cells infiltrating the trigeminal ganglia at day 6 post infection compared to sham-immunized mice. Significant differences were not seen in latent viral reservoir between immunized and unimmunized mouse groups. Immunization with gD-ASOR decreased the severity of acute ocular HSV-1 infection, induced a CD4(+) T cell response, decreased the viral load in the trigeminal ganglia, but did not diminish viral latency.
机译:在八周大的雌性BALB / c小鼠中评估了针对单纯疱疹病毒1(HSV-1)糖蛋白D(gD)的DNA疫苗的抗病毒作用。核酸酶不敏感构建体(gD-ASOR)由HSV-1 gD编码质粒组成,该质粒与无唾液酸类类脂质体(ASOR)偶联,将其靶向带有ASOR受体的细胞。在第0天和第7天用10微克剂量的gD-ASOR或对照物质免疫小鼠。 14天后,通过角膜途径用10(5)pfu或10(6)pfu HSV-1,菌株17syn +感染小鼠。与假免疫小鼠相比,在感染后21天的观察期内,免疫小鼠的眼部疾病严重程度显着降低。急性复制动力学分析表明,与假免疫小鼠相比,免疫BALB / c小鼠的三叉神经节第6天病毒滴度降低了100倍。与假免疫小鼠相比,在感染后第6天,免疫小鼠显示浸入三叉神经节的CD4(+)T细胞数量显着增加。免疫组和未免疫组之间在潜伏病毒库中未见明显差异。 gD-ASOR免疫降低了急性眼HSV-1感染的严重程度,诱导了CD4(+)T细胞反应,降低了三叉神经节中的病毒载量,但并未减少病毒潜伏期。

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