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B群2b型脑膜炎奈瑟菌蛋白疫苗的研制及在小鼠模型中的评价

Development of a Neisseria meningitidis group B serotype 2b protein vaccine and evaluation in a mouse model.

作者信息

Wang L Y, Frasch C E

出版信息

Infect Immun. 1984 Nov;46(2):408-14. doi: 10.1128/iai.46.2.408-414.1984.

Abstract

Although serotype 2 remains the predominant cause of group B Neisseria meningitidis disease in many parts of the world, most cases of this disease are now due to serotype 2b rather than 2a. For this reason, we adapted the serotype 2a vaccine method of C. E. Frasch and M. S. Peppler (Infect. Immun. 37:271-280, 1982) to the production of a serotype 2b protein vaccine. A spontaneously occurring nonencapsulated mutant of the group B serotype 2b strain 3006 was obtained by selection on group B antiserum agar. Serotype 2b outer membrane protein vaccines were prepared with less than 1% lipoplysaccharide contamination. The immunogenicity of these vaccines was evaluated in mice in the presence and absence of meningococcal group B and group C capsular polysaccharides. The group B and group C polysaccharides equally potentiated the antibody response to the serotype 2b protein. Addition of aluminum hydroxide or aluminum phosphate markedly improved the antibody response to the serotype 2b protein, but aluminum hydroxide-adjuvanted vaccines consistently elicited higher antibody levels. Aluminum hydroxide-adsorbed serotype 2a and 2b protein vaccines were evaluated for induction of cross-protective bactericidal antibodies. The 2a vaccines were 2a specific, whereas the 2b vaccines elicited antibodies strongly bactericidal for both 2a and 2b meningococcal strains and protected against bacteremia in a mouse model. It may therefore be possible to provide protection against both 2a and 2b disease by using an aluminum hydroxide-adsorbed protein vaccine containing a single serotype 2 protein component.

摘要

尽管血清型2仍是世界许多地区B群脑膜炎奈瑟菌病的主要病因,但现在这种疾病的大多数病例是由血清型2b而非2a引起的。因此,我们将C.E.弗拉施和M.S.佩普勒(《感染与免疫》37:271 - 280,1982年)的血清型2a疫苗制备方法应用于血清型2b蛋白疫苗的生产。通过在B群抗血清琼脂上筛选,获得了B群血清型2b菌株3006的一个自发产生的非包膜突变体。制备的血清型2b外膜蛋白疫苗脂多糖污染低于1%。在有和没有B群和C群脑膜炎球菌荚膜多糖存在的情况下,在小鼠中评估了这些疫苗的免疫原性。B群和C群多糖同样增强了对血清型2b蛋白的抗体反应。添加氢氧化铝或磷酸铝显著改善了对血清型2b蛋白的抗体反应,但氢氧化铝佐剂疫苗始终诱导出更高的抗体水平。评估了氢氧化铝吸附的血清型2a和2b蛋白疫苗诱导交叉保护性杀菌抗体的能力。2a疫苗具有2a特异性,而2b疫苗诱导出对2a和2b脑膜炎球菌菌株均具有强杀菌作用的抗体,并在小鼠模型中预防了菌血症。因此,使用含有单一血清型2蛋白成分的氢氧化铝吸附蛋白疫苗可能提供针对2a和2b疾病的保护。

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