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非人灵长类动物免疫接种引发的HIV-1交叉反应性原发性病毒中和抗体反应

HIV-1 Cross-Reactive Primary Virus Neutralizing Antibody Response Elicited by Immunization in Nonhuman Primates.

作者信息

Wang Yimeng, O'Dell Sijy, Turner Hannah L, Chiang Chi-I, Lei Lin, Guenaga Javier, Wilson Richard, Martinez-Murillo Paola, Doria-Rose Nicole, Ward Andrew B, Mascola John R, Wyatt Richard T, Karlsson Hedestam Gunilla B, Li Yuxing

机构信息

Institute for Bioscience and Biotechnology Research, University of Maryland, Rockville, Maryland, USA.

Department of Immunology and Microbial Science, The Scripps Research Institute, La Jolla, California, USA.

出版信息

J Virol. 2017 Oct 13;91(21). doi: 10.1128/JVI.00910-17. Print 2017 Nov 1.

Abstract

Elicitation of broadly neutralizing antibody (bNAb) responses is a major goal for the development of an HIV-1 vaccine. Current HIV-1 envelope glycoprotein (Env) vaccine candidates elicit predominantly tier 1 and/or autologous tier 2 virus neutralizing antibody (NAb) responses, as well as weak and/or sporadic cross-reactive tier 2 virus NAb responses with unknown specificity. To delineate the specificity of vaccine-elicited cross-reactive tier 2 virus NAb responses, we performed single memory B cell sorting from the peripheral blood of a rhesus macaque immunized with YU2gp140-F trimers in adjuvant, using JR-FL SOSIP.664, a native Env trimer mimetic, as a sorting probe to isolate monoclonal Abs (MAbs). We found striking genetic and functional convergence of the SOSIP-sorted Ig repertoire, with predominant VH4 or VH5 gene family usage and Env V3 specificity. Of these vaccine-elicited V3-specific MAbs, nearly 20% (6/33) displayed cross-reactive tier 2 virus neutralization, which recapitulated the serum neutralization capacity. Substantial similarities in binding specificity, neutralization breadth and potency, and sequence/structural homology were observed between selected macaque cross-reactive V3 NAbs elicited by vaccination and prototypic V3 NAbs derived from natural infections in humans, highlighting the convergence of this subset of primate V3-specific B cell repertories. Our study demonstrated that cross-reactive primary virus neutralizing B cell lineages could be elicited by vaccination as detected using a standardized panel of tier 2 viruses. Whether these lineages could be expanded to acquire increased breadth and potency of neutralization merits further investigation. Elicitation of antibody responses capable of neutralizing diverse HIV-1 primary virus isolates (designated broadly neutralizing antibodies [bNAbs]) remains a high priority for the vaccine field. bNAb responses were so far observed only in response to natural infection within a subset of individuals. To achieve this goal, an improved understanding of vaccine-elicited responses, including at the monoclonal Ab level, is essential. Here, we isolated and characterized a panel of vaccine-elicited cross-reactive neutralizing MAbs targeting the Env V3 loop that moderately neutralized several primary viruses and recapitulated the serum neutralizing antibody response. Striking similarities between the cross-reactive V3 NAbs elicited by vaccination in macaques and natural infections in humans illustrate commonalities between the vaccine- and infection-induced responses to V3 and support the feasibility of exploring the V3 epitope as a HIV-1 vaccine target in nonhuman primates.

摘要

诱导产生广泛中和抗体(bNAb)反应是HIV-1疫苗研发的主要目标。目前的HIV-1包膜糖蛋白(Env)候选疫苗主要诱导1级和/或自体2级病毒中和抗体(NAb)反应,以及微弱和/或散发性的具有未知特异性的交叉反应性2级病毒NAb反应。为了阐明疫苗诱导的交叉反应性2级病毒NAb反应的特异性,我们从用佐剂中的YU2gp140-F三聚体免疫的恒河猴外周血中进行单个记忆B细胞分选,使用天然Env三聚体模拟物JR-FL SOSIP.664作为分选探针来分离单克隆抗体(MAb)。我们发现SOSIP分选的Ig库在基因和功能上有显著的趋同,主要使用VH4或VH5基因家族且具有Env V3特异性。在这些疫苗诱导的V3特异性MAb中,近20%(6/33)表现出交叉反应性2级病毒中和作用,这概括了血清中和能力。在接种疫苗诱导的恒河猴交叉反应性V3 NAb与源自人类自然感染的原型V3 NAb之间,观察到结合特异性、中和广度和效力以及序列/结构同源性方面的实质性相似性,突出了灵长类V3特异性B细胞库这一子集的趋同。我们的研究表明,使用标准化的2级病毒组检测发现,接种疫苗可诱导交叉反应性原发性病毒中和B细胞谱系。这些谱系是否能够扩展以获得更大的中和广度和效力值得进一步研究。诱导能够中和多种HIV-1原发性病毒分离株的抗体反应(称为广泛中和抗体[bNAb])仍然是疫苗领域的高度优先事项。到目前为止,仅在一部分个体对自然感染的反应中观察到bNAb反应。为实现这一目标,更好地理解疫苗诱导的反应,包括在单克隆抗体水平上的理解,至关重要。在这里,我们分离并表征了一组针对Env V3环的疫苗诱导的交叉反应性中和MAb,它们能适度中和几种原发性病毒并概括了血清中和抗体反应。接种疫苗在恒河猴中诱导的交叉反应性V3 NAb与人类自然感染之间的显著相似性说明了疫苗诱导和感染诱导的针对V3的反应之间的共性,并支持在非人类灵长类动物中探索V3表位作为HIV-1疫苗靶点的可行性。

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