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HIV-1包膜糖蛋白免疫后揭示的多种抗体遗传和识别特性。

Diverse antibody genetic and recognition properties revealed following HIV-1 envelope glycoprotein immunization.

作者信息

Phad Ganesh E, Vázquez Bernat Néstor, Feng Yu, Ingale Jidnyasa, Martinez Murillo Paola Andrea, O'Dell Sijy, Li Yuxing, Mascola John R, Sundling Christopher, Wyatt Richard T, Karlsson Hedestam Gunilla B

机构信息

Department of Microbiology, Tumor and Cell Biology, Karolinska Institutet, 171 77 Stockholm, Sweden;

International AIDS Vaccine Initiative, Neutralizing Antibody Center, Department of Immunology and Microbial Science, The Scripps Research Institute, La Jolla, CA 92037;

出版信息

J Immunol. 2015 Jun 15;194(12):5903-14. doi: 10.4049/jimmunol.1500122. Epub 2015 May 11.

Abstract

Isolation of mAbs elicited by vaccination provides opportunities to define the development of effective immunity. Ab responses elicited by current HIV-1 envelope glycoprotein (Env) immunogens display narrow neutralizing activity with limited capacity to block infection by tier 2 viruses. Intense work in the field suggests that improved Env immunogens are forthcoming, and it is therefore important to concurrently develop approaches to investigate the quality of vaccine-elicited responses at a higher level of resolution. In this study, we cloned a representative set of mAbs elicited by a model Env immunogen in rhesus macaques and comprehensively characterized their genetic and functional properties. The mAbs were genetically diverse, even within groups of Abs targeting the same subregion of Env, consistent with a highly polyclonal response. mAbs directed against two subdeterminants of Env, the CD4 binding site and V region 3, could in part account for the neutralizing activity observed in the plasma of the animal from which they were cloned, demonstrating the power of mAb isolation for a detailed understanding of the elicited response. Finally, through comparative analyses of mAb binding and neutralizing capacity of HIV-1 using matched Envs, we demonstrate complex relationships between epitope recognition and accessibility, highlighting the protective quaternary packing of the HIV-1 spike relative to vaccine-induced mAbs.

摘要

通过疫苗接种引发的单克隆抗体(mAb)的分离为确定有效免疫的发展提供了机会。当前HIV-1包膜糖蛋白(Env)免疫原引发的抗体反应显示出狭窄的中和活性,阻断2级病毒感染的能力有限。该领域的大量研究表明,改进的Env免疫原即将出现,因此,同时开发在更高分辨率水平上研究疫苗引发反应质量的方法非常重要。在本研究中,我们克隆了恒河猴中由模型Env免疫原引发的一组代表性mAb,并全面表征了它们的遗传和功能特性。这些mAb在基因上具有多样性,即使在靶向Env同一亚区域的抗体组内也是如此,这与高度多克隆反应一致。针对Env的两个亚决定簇(CD4结合位点和V区3)的mAb可以部分解释在克隆它们的动物血浆中观察到的中和活性,证明了mAb分离对于详细了解引发反应的作用。最后,通过使用匹配的Env对HIV-1的mAb结合和中和能力进行比较分析,我们证明了表位识别与可及性之间的复杂关系,突出了HIV-1刺突相对于疫苗诱导的mAb的保护性四级结构。

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本文引用的文献

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Crystal structure of a soluble cleaved HIV-1 envelope trimer.可溶性 HIV-1 包膜三聚体的晶体结构
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