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The Plasmodium falciparum-Specific Human Memory B Cell Compartment Expands Gradually with Repeated Malaria Infections

机译:恶性疟原虫特异的人类记忆B细胞隔室随着反复的疟疾感染逐渐扩大

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摘要

Immunity to Plasmodium falciparum (Pf) malaria is only acquired after years of repeated infections and wanes rapidly without ongoing parasite exposure. Antibodies are central to malaria immunity, yet little is known about the B-cell biology that underlies the inefficient acquisition of Pf-specific humoral immunity. This year-long prospective study in Mali of 185 individuals aged 2 to 25 years shows that Pf-specific memory B-cells and antibodies are acquired gradually in a stepwise fashion over years of repeated Pf exposure. Both Pf-specific memory B cells and antibody titers increased after acute malaria and then, after six months of decreased Pf exposure, contracted to a point slightly higher than pre-infection levels. This inefficient, stepwise expansion of both the Pf-specific memory B-cell and long-lived antibody compartments depends on Pf exposure rather than age, based on the comparator response to tetanus vaccination that was efficient and stable. These observations lend new insights into the cellular basis of the delayed acquisition of malaria immunity.
机译:恶性疟原虫(Pf)疟疾的免疫力只有经过多年的反复感染才能获得,并且在没有持续的寄生虫暴露的情况下迅速消失。抗体是疟疾免疫力的核心,但对于导致无效获取Pf特异性体液免疫的B细胞生物学知之甚少。这项在马里进行的为期一年的前瞻性研究对2至25岁的185位个体进行了研究,结果表明,经过数年的反复暴露于Pf后,逐步逐步获得Pf特异性记忆B细胞和抗体。急性疟疾后,Pf特异性记忆B细胞和抗体滴度均增加,然后,在Pf暴露减少六个月后,收缩至略高于感染前水平的水平。 Pf特异性记忆B细胞和长寿命抗体区室的这种效率低下的逐步扩增取决于Pf的暴露量而不是年龄,这取决于比较者对破伤风疫苗接种的反应是有效且稳定的。这些观察为延迟获得疟疾免疫力的细胞基础提供了新的见解。

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