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结构分析一个登革热交叉反应抗体与包膜域 III 复合物揭示了交叉反应的分子基础。

Structural analysis of a dengue cross-reactive antibody complexed with envelope domain III reveals the molecular basis of cross-reactivity.

机构信息

Department of Medicine, Hammersmith Hospital Campus, Imperial College London, London W12 0NN, United Kingdom.

出版信息

J Immunol. 2012 May 15;188(10):4971-9. doi: 10.4049/jimmunol.1200227. Epub 2012 Apr 9.

Abstract

Dengue virus infections are still increasing at an alarming rate in tropical and subtropical countries, underlying the need for a dengue vaccine. Although it is relatively easy to generate Ab responses to dengue virus, low avidity or low concentrations of Ab may enhance infection of FcR-bearing cells with clinical impact, posing a challenge to vaccine production. In this article, we report the characterization of a mAb, 2H12, which is cross-reactive to all four serotypes in the dengue virus group. Crystal structures of 2H12-Fab in complex with domain III of the envelope protein from three dengue serotypes have been determined. 2H12 binds to the highly conserved AB loop of domain III of the envelope protein that is poorly accessible in the mature virion. 2H12 neutralization varied between dengue serotypes and strains; in particular, dengue serotype 2 was not neutralized. Because the 2H12-binding epitope was conserved, this variation in neutralization highlights differences between dengue serotypes and suggests that significant conformational changes in the virus must take place for Ab binding. Surprisingly, 2H12 facilitated little or no enhancement of infection. These data provide a structural basis for understanding Ab neutralization and enhancement of infection, which is crucial for the development of future dengue vaccines.

摘要

登革热病毒感染在热带和亚热带国家仍以惊人的速度持续增长,这凸显了对登革热疫苗的需求。虽然产生针对登革热病毒的 Ab 反应相对容易,但 Ab 的低亲和力或低浓度可能会增强具有临床影响的 FcR 携带细胞的感染,这给疫苗生产带来了挑战。在本文中,我们报告了一种 mAb(2H12)的特性,该 mAb 与登革热病毒组的所有四个血清型均发生交叉反应。已经确定了 2H12-Fab 与来自三种登革热血清型的包膜蛋白的结构域 III 复合物的晶体结构。2H12 结合到包膜蛋白结构域 III 的高度保守的 AB 环上,该环在成熟病毒粒子中不易接近。2H12 对登革热血清型和株之间的中和作用存在差异;特别是,登革热血清型 2 不能被中和。由于 2H12 的结合表位是保守的,这种中和作用的差异突出了登革热血清型之间的差异,并表明 Ab 结合必须发生重大的构象变化。令人惊讶的是,2H12 几乎没有或没有促进感染增强。这些数据为理解 Ab 中和作用和感染增强作用提供了结构基础,这对未来登革热疫苗的开发至关重要。

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