首页> 外文OA文献 >Antibody Profiling by Proteome Microarray Reveals the Immunogenicity of the Attenuated Smallpox Vaccine Modified Vaccinia Virus Ankara Is Comparable to That of Dryvax▿ †
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Antibody Profiling by Proteome Microarray Reveals the Immunogenicity of the Attenuated Smallpox Vaccine Modified Vaccinia Virus Ankara Is Comparable to That of Dryvax▿ †

机译:蛋白质组芯片的抗体分析揭示了天花减毒疫苗修饰的痘苗病毒安卡拉的免疫原性与Dryvax相当

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摘要

Modified vaccinia virus Ankara (MVA) is a highly attenuated vaccinia virus that is under consideration as an alternative to the conventional smallpox vaccine Dryvax. MVA was attenuated by extensive passage of vaccinia virus Ankara in chicken embryo fibroblasts. Several immunomodulatory genes and genes that influence host range are deleted or mutated, and replication is aborted in the late stage of infection in most nonavian cells. The effect of these mutations on immunogenicity is not well understood. Since the structural genes appear to be intact in MVA, it is hypothesized that critical targets for antibody neutralization have been retained. To test this, we probed microarrays of the Western Reserve (WR) proteome with sera from humans and macaques after MVA and Dryvax vaccination. As most protein sequences of MVA are 97 to 99% identical to those of other vaccinia virus strains, extensive binding cross-reactivity is expected, except for those deleted or truncated. Despite different hosts and immunization regimens, the MVA and Dryvax antibody profiles were broadly similar, with antibodies against membrane and core proteins being the best conserved. The responses to nonstructural proteins were less well conserved, although these are not expected to influence virus neutralization. The broadest antibody response was obtained for hyperimmune rabbits with WR, which is pathogenic in rabbits. These data indicate that, despite the mutations and deletions in MVA, its overall immunogenicity is broadly comparable to that of Dryvax, particularly at the level of antibodies to membrane proteins. The work supports other information suggesting that MVA may be a useful alternative to Dryvax.
机译:改良痘苗病毒安卡拉(MVA)是高度减毒的痘苗病毒,正在考虑替代常规天花疫苗Dryvax。牛痘病毒安卡拉在鸡胚成纤维细胞中的广泛传播减弱了MVA。一些感染调节基因和影响宿主范围的基因被删除或突变,并且在大多数非禽类细胞的感染后期复制被中止。这些突变对免疫原性的影响尚不清楚。由于结构基因在MVA中似乎是完整的,因此可以假设抗体中和的关键靶点已经保留。为了测试这一点,我们在接种MVA和Dryvax疫苗后,用人类和猕猴的血清探查了Western Reserve(WR)蛋白质组的微阵列。由于大多数MVA的蛋白质序列与其他痘苗病毒株的蛋白质序列具有97%到99%的相同性,因此,除了缺失或截断的序列,预期会有广泛的结合交叉反应性。尽管宿主和免疫方案不同,但MVA和Dryvax抗体谱大致相似,其中针对膜和核心蛋白的抗体最为保守。对非结构蛋白的反应保守性较低,尽管预计不会影响病毒中和。对于具有免疫原性的WR超免疫兔子,获得了最广泛的抗体应答。这些数据表明,尽管MVA发生了突变和缺失,但其总体免疫原性与Dryvax的免疫原性大致相当,特别是在针对膜蛋白的抗体水平上。该工作支持其他信息,表明MVA可能是Dryvax的有用替代品。

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