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首页> 外文期刊>Virology >Protection from genital herpes disease, seroconversion and latent infection in a non-lethal murine genital infection model by immunization with an HSV-2 replication-defective mutant virus
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Protection from genital herpes disease, seroconversion and latent infection in a non-lethal murine genital infection model by immunization with an HSV-2 replication-defective mutant virus

机译:通过用HSV-2复制缺陷突变病毒免疫,从生殖器疱疹病,血清转化和潜在感染血清鼠生殖器感染模型

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摘要

Viral vaccines have traditionally protected against disease, but for viruses that establish latent infection, it is desirable for the vaccine to reduce infection to reduce latent infection and reactivation. While seroconversion has been used in clinical trials of herpes simplex virus (HSV) vaccines to measure protection from infection, this has not been modeled in animal infection systems. To measure the ability of a genital herpes vaccine candidate to protect against various aspects of infection, we established a non-lethal murine model of genital HSV-2 infection, an ELISA assay to measure antibodies specific for infected cell protein 8 (ICP8), and a very sensitive qPCR assay. Using these assays, we observed that immunization with HSV-2 d15-29 virus reduced disease, viral shedding, seroconversion, and latent infection by the HSV-2 challenge virus. Therefore, it may be feasible to obtain protection against genital disease, seroconversion and latent infection by immunization, even if sterilizing immunity is not achieved. (C) 2015 Elsevier Inc. All rights reserved.
机译:病毒疫苗传统上保护免受疾病,但对于建立潜在感染的病毒,希望疫苗减少感染以降低潜在感染和再激活。虽然Seroconversion已用于疱疹病毒(HSV)疫苗的临床试验中,但从动物感染系统中尚未建模。为了测量生殖器疱疹疫苗候选人的能力,以防止感染的各个方面,我们建立了生殖器HSV-2感染的非致致致致致致致致致致致致致致致致致致致致偶的小鼠模型,以测量感染细胞蛋白8(ICP8)特异的抗体(ICP8)和一个非常敏感的QPCR测定。使用这些测定,我们观察到HSV-2 D15-29病毒免疫减少了疾病,病毒脱落,血清转化和受HSV-2攻击病毒的潜在感染。因此,即使未达到灭菌免疫,也可能是可行的免疫疾病,血清转化和潜伏感染可能是可行的。 (c)2015 Elsevier Inc.保留所有权利。

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