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A protein-based smallpox vaccine protects non-human primates from a lethal monkeypox virus challenge

机译:一种基于蛋白质的天花疫苗可保护非人类灵长类动物免受致命的猴痘病毒攻击

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摘要

Concerns about infections caused by orthopoxviruses, such as variola and monkeypox viruses, drive ongoing efforts to develop novel smallpox vaccines that are both effective and safe to use in diverse populations. A subunit smallpox vaccine comprising vaccinia virus membrane proteins A33,135, L1, A27 and aluminum hydroxide (alum)+/- CpG was administered to non-human primates, which were subsequently challenged with a lethal intravenous dose of monkeypox virus. Alum adjuvanted vaccines provided only partial protection but the addition of CpG provided full protection that was associated with a more homogeneous antibody response and stronger IgG1 responses. These results indicate that it is feasible to develop a highly effective subunit vaccine against orthopoxvirus infections as a safer alternative to live vaccinia virus vaccination. (c) 2010 Elsevier Ltd
机译:对由天花病毒(如天花和猴痘病毒)引起的感染的担忧,促使人们不断努力开发新型的天花疫苗,这种疫苗在不同人群中均有效且安全。将包含牛痘病毒膜蛋白A33,135,L1,A27和氢氧化铝(alum)+/- CpG的亚单位天花疫苗施用于非人类灵长类动物,随后用致死性静脉内剂量的猴痘病毒进行攻击。明矾佐剂疫苗仅提供部分保护,而添加CpG则提供了全面保护,这与更均一的抗体反应和更强的IgG1反应相关。这些结果表明,开发一种针对正痘病毒感染的高效亚单位疫苗是可行的,以替代活牛痘病毒疫苗。 (c)2010爱思唯尔有限公司

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