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首页> 外文期刊>Pharmaceuticals >Conformation and Cross-Protection in Group B Streptococcus Serotype III and Streptococcus pneumoniae Serotype 14: A Molecular Modeling Study
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Conformation and Cross-Protection in Group B Streptococcus Serotype III and Streptococcus pneumoniae Serotype 14: A Molecular Modeling Study

机译:B组链球菌血清型III和肺炎链球菌血清型14的构象和交叉保护:分子模型研究

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摘要

Although the branched capsular polysaccharides of Streptococcus agalactiae serotype III (GBSIII PS) and Streptococcus pneumoniae serotype 14 (Pn14 PS) differ only in the addition of a terminal sialic acid on the GBSIII PS side chains, these very similar polysaccharides are immunogenically distinct. Our simulations of GBSIII PS, Pn14 PS and the unbranched backbone polysaccharide provide a conformational rationale for the different antigenic epitopes identified for these PS. We find that side chains stabilize the proximal β d Glc(1→6) β d GlcNAc backbone linkage, restricting rotation and creating a well-defined conformational epitope at the branch point. This agrees with the glycotope structure recognized by an anti-GBSIII PS functional monoclonal antibody. We find the same dominant solution conformation for GBSIII and Pn14 PS: aside from the branch point, the backbone is very flexible with a “zig-zag” conformational habit, rather than the helix previously proposed for GBSIII PS. This suggests a common strategy for bacterial evasion of the host immune system: a flexible backbone that is less perceptible to the immune system, combined with conformationally-defined branch points presenting human-mimic epitopes. This work demonstrates how small structural features such as side chains can alter the conformation of a polysaccharide by restricting rotation around backbone linkages.
机译:尽管无乳链球菌血清型III(GBSIII PS)和肺炎链球菌血清型14(Pn14 PS)的分支荚膜多糖仅在GBSIII PS侧链上添加末端唾液酸有所不同,但这些非常相似的多糖在免疫学上是不同的。我们对GBSIII PS,Pn14 PS和直链主链多糖的模拟为这些PS鉴定出的不同抗原表位提供了构象基础。我们发现侧链稳定了近端βd Glc(1→6)βd GlcNAc主链,限制了旋转并在分支点形成了定义良好的构象表位。这与抗GBSIII PS功能性单克隆抗体识别的糖基结构相符。我们发现GBSIII和Pn14 PS具有相同的主导溶液构象:除分支点外,主链非常灵活,具有“ zig-zag”构象习惯,而不是先前为GBSIII PS提出的螺旋结构。这表明了逃避宿主免疫系统细菌的通用策略:免疫系统难以察觉的灵活骨架,结合呈现拟人抗原决定簇的构象定义分支点。这项工作证明了小的结构特征(如侧链)如何通过限制围绕骨架键的旋转来改变多糖的构象。

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