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首页> 外文期刊>Vaccine >Serotype of Streptococcus pneumoniae capsular polysaccharide can modifythe Th1/Th2 cytokine profile and IgG subclass response topneumococal-CRM197 conjugate vaccines in a murine model
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Serotype of Streptococcus pneumoniae capsular polysaccharide can modifythe Th1/Th2 cytokine profile and IgG subclass response topneumococal-CRM197 conjugate vaccines in a murine model

机译:肺炎链球菌荚膜多糖的血清型可以在鼠模型中修饰Th1 / Th2细胞因子谱和IgG亚类应答的Topneumococal-CRM197共轭疫苗

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The cellular and antibody responses to type 14 and type 19F Streptococcus pneumoniae capsular polysaccharides (PS) conjugated to CRM197 were investigated in a mouse model developed for pre-clinical evaluation and quality control of pneumococcal conjugate vaccines. Total IgG antibody and IgG subclasses against PS and the carrier protein for both conjugates were measured in addition to the T cell proliferation and cytokine profiles induced by these conjugates. While unconjugated PS 14 and 19F were at best only weakly immunogenic, both types of conjugate induced strong primary and secondary IgG responses to PS. The responses induced by the two conjugates to the carrier protein were very different; a high level of anti-CRM197 IgG was induced only by the PS19F conjugate whereas a very weak response was induced by the PS14 conjugate. Interestingly, the Ige subclass distribution was different for the two conjugates; for PS19F conjugate, the Ige response was almost completely of IgG1 subclass with low levels of IgG3 and IgG2a while the response to PS14 conjugate was mainly of the IgG1 and IgG2a subclasses with a low level of IgG3. The anti-CRM197 IgG subclass distribution was identical with that to the corresponding conjugated PS. Both types of conjugate induced strong T cell proliferation to recall antigens but induced different patterns of cytokine response in immune spleen cells which were indicative of a Th0 response or a mixture of Th1 and Th2 responses with a bias towards Th2 response in PS19F-CRM197 immunised mice. In conclusion, PS14- and PS19F-CRM197 conjugates induced different IgG subclass patterns as a result of inducing different patterns of cytokine response to the carrier protein. This indicates that the serotype of PS can modify the Th1/Th2 response to the carrier protein, which has a direct effect and can predict the IgG subclass of the PS response. Finally, we conclude that this model appears suitable for studying the immunogenicity and immune interaction of different components of multivalent pneumococcal conjugate vaccines and may be applicable to their pre-clinical evaluation and quality control.
机译:在为肺炎球菌结合疫苗的临床前评估和质量控制而开发的小鼠模型中,研究了与CRM197结合的14型和19F型19F肺炎链球菌荚膜多糖(PS)的细胞和抗体应答。除了这些缀合物诱导的T细胞增殖和细胞因子谱外,还测量了针对两种缀合物的PS和载体蛋白的总IgG抗体和IgG亚类。尽管未缀合的PS 14和19F充其量仅是弱免疫原性,但两种类型的缀合物均诱导对PS的强烈一级和二级IgG反应。两种结合物诱导的对载体蛋白的反应是非常不同的。仅PS19F缀合物诱导了高水平的抗CRM197 IgG,而PS14缀合物则诱导了非常弱的应答。有趣的是,两种缀合物的Ige子类分布是不同的。对于PS19F缀合物,Ige反应几乎完全是IgG1和IgG2a水平低的IgG1亚类,而对PS14缀合物的响应主要是IgG3和IgG3水平低的IgG1和IgG2a亚类。抗CRM197 IgG亚类分布与相应的缀合PS相同。两种类型的结合物均诱导强T细胞增殖以召回抗原,但在免疫脾细胞中诱导不同的细胞因子反应模式,这表明在PS19F-CRM197免疫小鼠中Th0反应或Th1和Th2反应的混合物偏向Th2反应。总之,由于诱导了针对载体蛋白的细胞因子应答的不同模式,PS14-和PS19F-CRM197共轭物诱导了不同的IgG亚类模式。这表明PS的血清型可以改变对载体蛋白的Th1 / Th2应答,这具有直接的作用并且可以预测PS应答的IgG亚类。最后,我们得出结论,该模型似乎适合研究多价肺炎球菌结合疫苗不同成分的免疫原性和免疫相互作用,并且可能适用于其临床前评估和质量控制。

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