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The Blood-Stage Malaria Antigen PfRH5 is Susceptible to Vaccine-Inducible Cross-Strain Neutralizing Antibody

机译:血液阶段疟疾抗原PfRH5对疫苗诱导的交叉菌株中和抗体敏感

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摘要

Current vaccine strategies against the asexual blood-stage of Plasmodium falciparum are mostly focused on well-studied merozoite antigens which induce immune responses after natural exposure, but have yet to induce robust protection in any clinical trial. Here we compare human-compatible viral vectored vaccines targeting ten different blood-stage antigens. We show that the full-length P. falciparum reticulocyte-binding protein homologue 5 (PfRH5) is highly susceptible to cross-strain neutralizing vaccine-induced antibodies, out-performing all other antigens delivered by the same vaccine platform. We find that despite being susceptible to antibody, PfRH5 is unlikely to be under substantial immune selection pressure; there is minimal acquisition of anti-PfRH5 IgG antibodies in malaria-exposed Kenyans. These data challenge the widespread beliefs that any merozoite antigen that is highly susceptible to immune attack would be subject to significant levels of antigenic polymorphism, and that erythrocyte invasion by P. falciparum is a degenerate process involving a series of parallel redundant pathways.
机译:当前针对恶性疟原虫无血期的疫苗策略主要集中在经过充分研究的裂殖子抗原上,该抗原可在自然暴露后诱导免疫反应,但尚未在任何临床试验中诱导出强有力的保护作用。在这里,我们比较了针对人的兼容病毒载体疫苗,这些疫苗针对的是十种不同的血液阶段抗原。我们显示,全长恶性疟原虫网状细胞结合蛋白同源物5(PfRH5)对交叉株中和疫苗诱导的抗体高度敏感,胜过由同一疫苗平台提供的所有其他抗原。我们发现,尽管PfRH5容易受到抗体的影响,但它不太可能承受较大的免疫选择压力。在暴露于疟疾的肯尼亚人中,抗PfRH5 IgG抗体的获得极少。这些数据挑战了普遍的观念,即任何高度易受免疫攻击的裂殖子抗原都将遭受显着水平的抗原多态性,并且恶性疟原虫侵袭红细胞是简并过程,涉及一系列平行的冗余途径。

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