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肺炎球菌10型荚膜多糖分子构象的建模为表位和观察到的交叉反应性提供了深入了解。

Modeling of pneumococcal serogroup 10 capsular polysaccharide molecular conformations provides insight into epitopes and observed cross-reactivity.

作者信息

Richardson Nicole I, Kuttel Michelle M, Ravenscroft Neil

机构信息

Department of Chemistry, University of Cape Town, Cape Town, South Africa.

Department of Computer Science, University of Cape Town, Cape Town, South Africa.

出版信息

Front Mol Biosci. 2022 Aug 8;9:961532. doi: 10.3389/fmolb.2022.961532. eCollection 2022.

Abstract

is an encapsulated gram-negative bacterium and a significant human pathogen The capsular polysaccharide (CPS) is essential for virulence and a target antigen for vaccines. Although widespread introduction of pneumococcal conjugate vaccines (PCVs) has significantly reduced disease, the prevalence of non-vaccine serotypes has increased. On the basis of the CPS, serogroup 10 comprises four main serotypes 10A, 10B, 10C, and 10F; as well as the recently identified 10D. As it is the most prevalent, serotype 10A CPS has been included as a vaccine antigen in the next generation PCVs. Here we use molecular modeling to provide conformational rationales for the complex cross-reactivity reported between serotypes 10A, 10B, 10C, and 10F anti-sera. Although the highly mobile phosphodiester linkages produce very flexible CPS, shorter segments are conformationally defined, with exposed -D-galactofuranose ( DGal) side chains that are potential antibody binding sites. We identify four distinct conformational epitopes for the immunodominant DGal that assist in rationalizing the complex asymmetric cross-reactivity relationships. In particular, we find that strongly cross-reactive serotypes share common epitopes. Further, we show that human intelectin-1 has the potential to bind the exposed exocyclic 1,2-diol of the terminal DGal in each serotype; the relative accessibility of three- or six-linked DGal may play a role in the strength of the innate immune response and hence serotype disease prevalence. In conclusion, our modeling study and relevant serological studies support the inclusion of serotype 10A in a vaccine to best protect against serogroup 10 disease.

摘要

是一种包膜革兰氏阴性菌,也是一种重要的人类病原体。荚膜多糖(CPS)对致病性至关重要,是疫苗的靶抗原。尽管广泛引入肺炎球菌结合疫苗(PCV)已显著减少疾病,但非疫苗血清型的流行率有所增加。基于CPS,血清群10包括四种主要血清型10A、10B、10C和10F;以及最近鉴定出的10D。由于血清型10A是最常见的,其CPS已被纳入下一代PCV的疫苗抗原中。在这里,我们使用分子建模为血清型10A、10B、10C和10F抗血清之间报道的复杂交叉反应提供构象原理。尽管高度可移动的磷酸二酯键产生了非常灵活的CPS,但较短的片段在构象上是确定的,具有暴露的α-D-半乳呋喃糖(α-DGal)侧链,这些侧链是潜在的抗体结合位点。我们为免疫显性的α-DGal确定了四个不同的构象表位,有助于解释复杂的不对称交叉反应关系。特别是,我们发现强交叉反应血清型共享共同表位。此外,我们表明人类intlectin-1有可能结合每种血清型中末端α-DGal暴露的环外1,2-二醇;三连接或六连接α-DGal的相对可及性可能在先天免疫反应强度以及血清型疾病流行率中起作用。总之,我们的建模研究和相关血清学研究支持将血清型10A纳入疫苗,以最佳地预防血清群10疾病。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3699/9393222/e23c086ed497/fmolb-09-961532-g001.jpg

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