Lymphocyte Interaction Laboratory, Francis Crick Institute, London, England, UK.
Ragon Institute of Massachusetts General Hospital, MIT, and Harvard, Cambridge, MA.
J Exp Med. 2017 Aug 7;214(8):2471-2490. doi: 10.1084/jem.20170633.
Vaccines remain the most effective tool to prevent infectious diseases. Here, we introduce an in vitro booster vaccination approach that relies on antigen-dependent activation of human memory B cells in culture. This stimulation induces antigen-specific B cell proliferation, differentiation of B cells into plasma cells, and robust antibody secretion after a few days of culture. We validated this strategy using cells from healthy donors to retrieve human antibodies against tetanus toxoid and influenza hemagglutinin (HA) from H1N1 and newly emergent subtypes such as H5N1 and H7N9. Anti-HA antibodies were cross-reactive against multiple subtypes, and some showed neutralizing activity. Although these antibodies may have arisen as a result of previous influenza infection, we also obtained gp120-reactive antibodies from non-HIV-infected donors, indicating that we can generate antibodies without prior antigenic exposure. Overall, our novel approach can be used to rapidly produce therapeutic antibodies and has the potential to assess the immunogenicity of candidate antigens, which could be exploited in future vaccine development.
疫苗仍然是预防传染病最有效的工具。在这里,我们介绍了一种体外增强疫苗接种方法,该方法依赖于在培养物中抗原依赖性激活人记忆 B 细胞。这种刺激可诱导抗原特异性 B 细胞增殖、B 细胞分化为浆细胞,并在培养几天后产生强烈的抗体分泌。我们使用来自健康供体的细胞验证了该策略,从破伤风类毒素和甲型流感血凝素 (HA) 中检索针对 H1N1 以及新出现的亚型(如 H5N1 和 H7N9)的人抗体。抗-HA 抗体与多种亚型具有交叉反应性,有些具有中和活性。尽管这些抗体可能是由于先前的流感感染而产生的,但我们还从非 HIV 感染的供体中获得了 gp120 反应性抗体,表明我们可以在没有先前抗原暴露的情况下产生抗体。总的来说,我们的新方法可用于快速生产治疗性抗体,并有可能评估候选抗原的免疫原性,这可用于未来的疫苗开发。
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