首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Structures of synthetic O-antigen fragments from serotype 2a Shigella flexneri in complex with a protective monoclonal antibody
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Structures of synthetic O-antigen fragments from serotype 2a Shigella flexneri in complex with a protective monoclonal antibody

机译:血清型2a志贺氏志贺氏菌与保护性单克隆抗体复合的合成O抗原片段的结构

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摘要

The anti-LPS IgG mAb F22-4, raised against Shigella flexneri serotype 2a bacteria, protects against homologous, but not heterologous, challenge in an experimental animal model. We report the crystal structures of complexes formed between Fab F22-4 and two synthetic oligosaccharides, a decasaccharide and a pentadecasaccharide that were previously shown to be both immunogenic and antigenic mimics of the S. flexneri serotype 2a O-antigen. F22-4 binds to an epitope contained within two consecutive 2a serotype pentasaccharide repeat units (RU). Six sugar residues from a contiguous nine-residue segment make direct contacts with the antibody, including the nonreducing rhamnose and both branching glucosyl residues from the two RUs. The glucosyl residue, whose position of attachment to the tetrasaccharide backbone of the RU defines the serotype 2a O-antigen, is critical for recognition by F22-4. Although the complete decasaccharide is visible in the electron density maps, the last four pentadecasaccharide residues from the reducing end, which do not contact the antibody, could not be traced. Although considerable mobility in the free oligosaccharides can thus be expected, the conformational similarity between the individual RUs, both within and between the two complexes, suggests that short-range transient ordering to a helical conformation might occur in solution. Although the observed epitope includes the terminal nonreducing residue, binding to internal epitopes within the polysaccharide chain is not precluded. Our results have implications for vaccine development because they suggest that a minimum of two RUs of synthetic serotype 2a oligosaccharide is required for optimal mimicry of O-Ag epitopes.
机译:针对弗氏志贺氏菌血清型2a细菌产生的抗LPS IgG mAb F22-4,可抵抗实验动物模型中的同源但非异源攻击。我们报告了Fab F22-4与两个合成的寡糖,十糖和十五糖之间形成的复合物的晶体结构,先前显示它们是弗氏链球菌血清型2a O抗原的免疫原性和抗原性模仿物。 F22-4与两个连续的2a血清型五糖重复单元(RU)中包含的表位结合。来自连续九个残基区段的六个糖残基与抗体直接接触,包括非还原鼠李糖和来自两个RU的两个分支糖基残基。葡萄糖基残基的位置与RU的四糖骨架相连,定义了血清型2a O-抗原,对于F22-4的识别至关重要。尽管在电子密度图中可以看到完整的十糖,但无法追踪到还原端的最后四个未与抗体接触的十五糖残基。尽管因此可以预期游离寡糖具有相当大的迁移率,但是两个复合物中以及两个复合物之间的单个RU之间的构象相似性表明,溶液中可能会发生短时瞬态有序的螺旋构象。尽管观察到的表位包括末端非还原性残基,但不排除与多糖链内的内部表位结合。我们的结果对疫苗的开发具有重要意义,因为它们表明,对于O-Ag表位的最佳模拟,至少需要两个RU的合成血清型2a寡糖。

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