Immune response and protective efficacy of S9 ribosomal protein of Streptococcus pneumoniae in a model of sepsis

免疫原性 肺炎链球菌 核糖体蛋白 微生物学 生物 免疫系统 抗体 抗原 重组DNA 接种疫苗 病毒学 基因 免疫学 核糖体 抗生素 生物化学 核糖核酸
作者
Helton Fernandes Araújo,Paulo Henrique Almeida Campos-Junior,Dhian Renato Almeida Camargo,Filippe Nonato Roberto Pereira,Michelle Lara Samuel,Marluce Aparecida Assunção Oliveira,Consuelo Latorre Fortes-Dias,Sophie Leclercq
出处
期刊:Canadian Journal of Microbiology [Canadian Science Publishing]
卷期号:58 (9): 1055-1062 被引量:6
标识
DOI:10.1139/w2012-083
摘要

Vaccination is the most promising strategy to reduce the incidence of pneumococcal infection. Although there are vaccines available, all of them are based on polysaccharide antigens (conjugated or not). In addition to their high cost, those vaccines do not cover all serotypes. To overcome these hindrances, we evaluated the immunogenicity and the protective efficacy of the S9 ribosomal protein of Streptococcus pneumoniae with the aim of developing a protein-based vaccine in the future. The gene encoding the S9 ribosomal protein was cloned in pET21-a expression vector, and the recombinant S9 protein was used to immunize mice. Significantly higher levels of anti-S9 immunoglobulin G were achieved (with predominance of immunoglobulin G1) in comparison with the control. Antibodies elicited against S. pneumoniae protein extract in rabbit recognized the recombinant S9 protein by Western blot, thus demonstrating its immunogenicity. Moreover, mice immunized with recombinant S9 protein and challenged with a virulent strain of S. pneumoniae presented a significant reduction of bacteremia after 24 h of infection as compared with the control. However, in the S9-immunized mice the onset of death was insignificantly delayed, but all of them died by the fourth day postinfection.
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