Rescuing pathogen-specific memory B-cell from PBMC of prior Zika virus-infected individuals

IF 3.3 4区医学 Q3 IMMUNOLOGY Immunology letters Pub Date : 2024-11-12 DOI:10.1016/j.imlet.2024.106944

Jacyelle Medeiros Silva , Renato Kaylan Alves de Oliveira França , Pedro Henrique Barros , Hitallo Guilherme Costa Fontinele , Simone Gonçalves Fonseca , Marcelo Macedo Brigido , Andrea Queiroz Maranhão

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Abstract

Immunological memory, a fundamental immune system mechanism, is instrumental in long-term protection. Successful vaccines can elicit and sustain immunological memory against pathogens for the long term. Memory B cells (MBC) are key players in secondary responses due to their longevity and rapid differentiation into high-affinity antibody-secreting cells upon second antigen exposure. However, the availability of circulating MBCs is limited. Here we describe a protocol, which presents a straightforward and practical method for activating and expanding Zika virus (ZIKV) specific MBC. PBMCs collected from individuals who had been infected with ZIKV two years prior were cultured by supplementing with IL-2 and R848, a TLR-7/8 agonist, and then pulsed with inactivated virus. After seven days, this stimulation led to a notable rise in virus-specific functional MBC, as evidenced by a significant increase in the production of anti-ZIKV IgG. Importantly, the ZIKV pulse did not induce changes in the PBMC culture of individuals without a history of ZIKV infection. These findings demonstrate that virus-specific MBC can be expanded in vitro, even using PBMC cultures from individuals infected years before. Therefore, our protocol is a practical and effective tool for studies that require a larger number of human MBCs from previously infected individuals that are functional and specific to the pathogen under investigation.

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从寨卡病毒感染者的 PBMC 中拯救病原体特异性记忆 B 细胞。

免疫记忆是免疫系统的一种基本机制，对长期保护至关重要。成功的疫苗可以激发并维持针对病原体的长期免疫记忆。记忆 B 细胞（MBC）寿命长，并且在第二次接触抗原时能迅速分化为高亲和性抗体分泌细胞，因此是次级反应的关键因素。然而，循环 MBC 的可用性有限。在此，我们介绍了一种激活和扩增寨卡病毒（ZIKV）特异性 MBC 的直接而实用的方法。通过补充 IL-2 和 TLR-7/8 激动剂 R848 来培养从两年前感染过 ZIKV 的人身上收集的 PBMC，然后用灭活病毒进行脉冲刺激。七天后，这种刺激导致病毒特异性功能性 MBC 明显增加，抗 ZIKV IgG 的产生显著增加就是证明。重要的是，ZIKV 脉冲不会诱导无 ZIKV 感染史的个体的 PBMC 培养发生变化。这些研究结果表明，病毒特异性 MBC 可以在体外扩增，即使使用的是多年前感染者的 PBMC 培养物。因此，我们的方案是一种实用而有效的工具，适用于需要从先前感染者那里获得更多具有功能性和对所研究病原体特异性的人类 MBC 的研究。

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来源期刊

Immunology letters 医学-免疫学

CiteScore

7.60

自引率

0.00%

发文量

审稿时长

44 days

期刊介绍： Immunology Letters provides a vehicle for the speedy publication of experimental papers, (mini)Reviews and Letters to the Editor addressing all aspects of molecular and cellular immunology. The essential criteria for publication will be clarity, experimental soundness and novelty. Results contradictory to current accepted thinking or ideas divergent from actual dogmas will be considered for publication provided that they are based on solid experimental findings. Preference will be given to papers of immediate importance to other investigators, either by their experimental data, new ideas or new methodology. Scientific correspondence to the Editor-in-Chief related to the published papers may also be accepted provided that they are short and scientifically relevant to the papers mentioned, in order to provide a continuing forum for discussion.