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侵袭性脑膜炎奈瑟菌分离株中因子 H 结合蛋白模块群的频率和交叉反应杀菌活性的易感性。

Frequency of factor H-binding protein modular groups and susceptibility to cross-reactive bactericidal activity in invasive meningococcal isolates.

机构信息

Center for Immunobiology and Vaccine Development, Children's Hospital Oakland Research Institute, 5700 Martin Luther King Jr. Way, Oakland, CA 94609, USA.

出版信息

Vaccine. 2010 Feb 25;28(9):2122-9. doi: 10.1016/j.vaccine.2009.12.027. Epub 2009 Dec 29.

DOI:10.1016/j.vaccine.2009.12.027
PMID:20044056
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2830318/
Abstract

Meningococcal factor H-binding protein (fHbp) is a promising vaccine candidate that elicits serum bactericidal antibodies in humans. Based on sequence variability of the entire protein, fHbp has been divided into three variant groups or two sub-families. We recently reported that the fHbp architecture was modular, consisting of five variable segments, each encoded by genes from one of two lineages. Based on combinations of segments from different lineages, all 70 known fHbp sequence variants could be classified into one of six modular groups. In this study, we analyzed sequences of 172 new fHbp variants that were available from public databases. All but three variants could be classified into one of the six previously described modular groups. Among systematically collected invasive group B isolates from the U.S. and Europe, modular group I overall was most common (60%) but group IV (natural chimeras) accounted for 23% of UK isolates and <1% of U.S. isolates (P<0.0001). Mouse antisera to recombinant fHbp from each of the modular groups showed modular group-specific bactericidal activity against strains with low fHbp expression but had broader activity against strains with higher fHbp expression. Thus both modular group and relative expression of fHbp affected strain susceptibility to anti-fHbp bactericidal activity. The results confirmed the modular architecture of fHbp and underscored its importance for the design of broadly protective group B vaccines in different regions.

摘要

脑膜炎奈瑟菌因子 H 结合蛋白(fHbp)是一种很有前途的疫苗候选物,能在人体内诱导血清杀菌抗体。基于整个蛋白的序列变异性,fHbp 已被分为三个变异组或两个亚家族。我们最近报道称,fHbp 结构具有模块性,由五个可变片段组成,每个片段由来自两个谱系之一的基因编码。基于不同谱系片段的组合,所有已知的 70 种 fHbp 序列变体可分为六个模块组之一。在这项研究中,我们分析了来自公共数据库的 172 种新 fHbp 变体的序列。除了三种变体之外,所有变体都可以归入之前描述的六个模块组之一。在系统性收集的来自美国和欧洲的侵袭性 B 组分离株中,总体上模块组 I 最为常见(60%),但模块组 IV(天然嵌合体)占英国分离株的 23%,占美国分离株的不到 1%(P<0.0001)。针对每个模块组的重组 fHbp ,小鼠抗血清对低表达 fHbp 的菌株具有特定于模块组的杀菌活性,但对高表达 fHbp 的菌株具有更广泛的活性。因此,fHbp 的模块组和相对表达都影响了菌株对抗 fHbp 杀菌活性的敏感性。研究结果证实了 fHbp 的模块化结构,并强调了其在不同地区设计广泛保护性 B 组疫苗中的重要性。

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本文引用的文献

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