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用细胞表面蛋白Rib和α的高度纯化制剂对B族链球菌(一种有荚膜的细菌)进行实验性疫苗接种。

Experimental vaccination against group B streptococcus, an encapsulated bacterium, with highly purified preparations of cell surface proteins Rib and alpha.

作者信息

Larsson C, Stålhammar-Carlemalm M, Lindahl G

机构信息

Department of Medical Microbiology, Lund University, Sweden.

出版信息

Infect Immun. 1996 Sep;64(9):3518-23. doi: 10.1128/iai.64.9.3518-3523.1996.

Abstract

Encapsulated bacteria cause some of the most common diseases in humans. Although the polysaccharide capsules of these pathogens have attracted the most attention with regard to vaccine development, recent evidence suggests that bacterial surface proteins may also be used to confer protective immunity. We have analyzed this possibility in group B streptococcus (GBS), an encapsulated bacterium that is the major cause of invasive bacterial disease in the neonatal period. Previous work has shown that the majority of GBS strains causing invasive infections express the Rib protein, and that most strains lacking Rib express a protein designated alpha. Here we report that active immunization with highly purified preparations of Rib or alpha protected mice against lethal infection with strains expressing the corresponding protein. Vaccination with the Rib protein protected against two strains of capsular type III and two strains of type II, and vaccination with the alpha protein protected against one strain of type II and one strain of type Ib. The mice vaccinated with Rib or alpha showed a good immunoglobulin G response to the immunogen. These data suggest that a vaccine against GBS disease may be based on cell surface proteins and support the notion that proteins may be used for immunization against encapsulated bacteria.

摘要

包膜细菌可引发人类一些最常见的疾病。尽管这些病原体的多糖包膜在疫苗研发方面最受关注,但最近的证据表明,细菌表面蛋白也可用于赋予保护性免疫。我们已在B族链球菌(GBS)中分析了这种可能性,GBS是一种包膜细菌,是新生儿期侵袭性细菌疾病的主要病因。先前的研究表明,大多数引起侵袭性感染的GBS菌株表达Rib蛋白,而大多数缺乏Rib的菌株表达一种名为α的蛋白。在此我们报告,用高度纯化的Rib或α制剂进行主动免疫可保护小鼠免受表达相应蛋白的菌株的致死性感染。用Rib蛋白进行疫苗接种可抵御两株III型荚膜菌株和两株II型菌株,用α蛋白进行疫苗接种可抵御一株II型菌株和一株Ib型菌株。接种Rib或α的小鼠对免疫原表现出良好的免疫球蛋白G反应。这些数据表明,针对GBS疾病的疫苗可能基于细胞表面蛋白,并支持蛋白可用于针对包膜细菌进行免疫的观点。

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