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壳蛋白缺失突变致弱的西尼罗河病毒活疫苗候选株的鉴定。

Characterization of West Nile virus live vaccine candidates attenuated by capsid deletion mutations.

机构信息

Intercell AG, Campus Vienna Biocenter 3, Vienna, Austria.

出版信息

Vaccine. 2010 Aug 16;28(36):5903-9. doi: 10.1016/j.vaccine.2010.06.045. Epub 2010 Jun 25.

Abstract

Protein C deletion mutants of West Nile virus (WNV) were evaluated for their potential use as live virus vaccine candidates in vivo. Double and triple mutants carrying small deletions and second-site point mutations, as well as mutants with large deletions of 36 and 37 amino acid residues were tested in a stringent mouse challenge model. The mutant viruses were found to be non-pathogenic and to induce protective immunity in a wide range of inoculation doses (10(1)-10(6)FFU). Furthermore, the effects of combining three different previously identified resuscitating point mutations, as well as the combination of a large protein C deletion with a deletion mutation in the 3' non-coding region were studied. The data indicate that the production of safe and efficacious WNV live vaccines based on protein C deletion mutations is feasible.

摘要

西尼罗河病毒(WNV)的蛋白 C 缺失突变体被评估为体内使用的活病毒候选疫苗。携带小缺失和第二位置点突变的双突变体和三突变体,以及具有 36 和 37 个氨基酸残基的大缺失突变体在严格的小鼠挑战模型中进行了测试。突变病毒被发现无致病性,并在广泛的接种剂量(10(1)-10(6)FFU)下诱导保护性免疫。此外,还研究了三种先前确定的复活点突变的组合,以及蛋白 C 缺失与 3'非编码区缺失突变的组合的效果。数据表明,基于蛋白 C 缺失突变生产安全有效的 WNV 活疫苗是可行的。

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