用艾滋病毒包膜三聚体免疫奶牛,可产生针对超长 CDRH3 复合物中 V2-apex 的广泛中和抗体

IF 6.7 1区 医学 Q1 Immunology and Microbiology
Pilar X. Altman, Gabriel Ozorowski, Robyn L. Stanfield, Jeremy Haakenson, Michael Appel, Mara Parren, Wen-Hsin Lee, Huldah Sang, Jordan Woehl, Karen Saye-Francisco, Leigh M. Sewall, Collin Joyce, Ge Song, Katelyn Porter, Elise Landais, Raiees Andrabi, Ian A. Wilson, Andrew B. Ward, Waithaka Mwangi, Vaughn V. Smider, Dennis R. Burton, Devin Sok
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引用次数: 0

摘要

针对 HIV 包膜(Env)上的保守表位产生广泛中和抗体(bnAbs)是 HIV 疫苗研究的基石之一。常用的 HIV 动物模型不能可靠地产生有效的广谱中和血清抗体反应,但奶牛除外。以前,奶牛曾通过同源质粒和类本地 Env 三聚体增强产生 CD4 结合位点反应。在小动物模型中,其他工程免疫原被证明能使抗体反应集中到 Env 的 bnAb V2-apex 区域。在这里,我们用两种V2-apex集中Env免疫原免疫两组奶牛(n = 4),以研究是否能产生针对Env上V2-apex的抗体反应。第 1 组使用黑猩猩猿猴免疫缺陷病毒(SIV)-Env 三聚体(与 HIV 共享 V2-apex)进行免疫,然后使用 C108(V2-apex 聚焦免疫原)进行免疫,最后使用交叉支链本地样三聚体鸡尾酒进行强化。纵向血清分析表明,每组中都有一头牛产生了针对 V2-apex 的血清中和抗体反应。从第 1 组和第 2 组奶牛中分别分离出 8 种和 11 种 bnAbs,并显示出适度的广泛性和效力。这项研究中的强效和广泛反应比以前的奶牛免疫晚得多,以前的奶牛免疫会引起 CD4bs bnAbs 反应,而且需要几种不同的免疫原。所有分离出的 bnAbs 都来自超长 CDRH3 序列。奶牛抗体可以针对 HIV 表面一个以上的广谱中和表位,这一发现揭示了细长结构在识别高度糖基化蛋白质方面的普遍性。尽管超长 CDRH3 bnAbs 只占奶牛抗体库的一小部分,但它们的独家分离结果表明,在 bnAb 反应过程中,这些抗体会取代长 CDRH3 和短 CDRH3 抗体。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Immunization of cows with HIV envelope trimers generates broadly neutralizing antibodies to the V2-apex from the ultralong CDRH3 repertoire
The generation of broadly neutralizing antibodies (bnAbs) to conserved epitopes on HIV Envelope (Env) is one of the cornerstones of HIV vaccine research. The animal models commonly used for HIV do not reliably produce a potent broadly neutralizing serum antibody response, with the exception of cows. Cows have previously produced a CD4 binding site response by homologous prime and boosting with a native-like Env trimer. In small animal models, other engineered immunogens were shown to focus antibody responses to the bnAb V2-apex region of Env. Here, we immunized two groups of cows (n = 4) with two regimens of V2-apex focusing Env immunogens to investigate whether antibody responses could be generated to the V2-apex on Env. Group 1 was immunized with chimpanzee simian immunodeficiency virus (SIV)-Env trimer that shares its V2-apex with HIV, followed by immunization with C108, a V2-apex focusing immunogen, and finally boosted with a cross-clade native-like trimer cocktail. Group 2 was immunized with HIV C108 Env trimer followed by the same HIV trimer cocktail as Group 1. Longitudinal serum analysis showed that one cow in each group developed serum neutralizing antibody responses to the V2-apex. Eight and 11 bnAbs were isolated from Group 1 and Group 2 cows, respectively, and showed moderate breadth and potency. Potent and broad responses in this study developed much later than previous cow immunizations that elicited CD4bs bnAbs responses and required several different immunogens. All isolated bnAbs were derived from the ultralong CDRH3 repertoire. The finding that cow antibodies can target more than one broadly neutralizing epitope on the HIV surface reveals the generality of elongated structures for the recognition of highly glycosylated proteins. The exclusive isolation of ultralong CDRH3 bnAbs, despite only comprising a small percent of the cow repertoire, suggests these antibodies outcompete the long and short CDRH3 antibodies during the bnAb response.
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来源期刊
PLoS Pathogens
PLoS Pathogens 生物-病毒学
CiteScore
11.40
自引率
3.00%
发文量
598
审稿时长
2 months
期刊介绍: Bacteria, fungi, parasites, prions and viruses cause a plethora of diseases that have important medical, agricultural, and economic consequences. Moreover, the study of microbes continues to provide novel insights into such fundamental processes as the molecular basis of cellular and organismal function.
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