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Structural basis for recognition of the malaria vaccine candidate Pfs48/45 by a transmission blocking antibody

机译:传播阻断抗体识别疟疾候选疫苗Pfs48 / 45的结构基础

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The quest to develop an effective malaria vaccine remains a major priority in the fight against global infectious disease. An approach with great potential is a transmission-blocking vaccine which induces antibodies that prevent establishment of a productive infection in mosquitos that feed on infected humans, thereby stopping the transmission cycle. One of the most promising targets for such a vaccine is the gamete surface protein, Pfs48/45. Here we establish a system for production of full-length Pfs48/45 and use this to raise a panel of monoclonal antibodies. We map the binding regions of these antibodies on Pfs48/45 and correlate the location of their epitopes with their transmission-blocking activity. Finally, we present the structure of the C-terminal domain of Pfs48/45 bound to the most potent transmission-blocking antibody, and provide key molecular information for future structure-guided immunogen design.
机译:寻求开发有效的疟疾疫苗仍然是抗击全球传染病的主要优先事项。一种具有巨大潜力的方法是一种阻断传播的疫苗,该疫苗可诱导可防止在以受感染的人类为食的蚊子中建立生产性感染的抗体,从而终止传播周期。这种疫苗最有希望的靶标之一是配子表面蛋白Pfs48 / 45。在这里,我们建立了用于生产全长Pfs48 / 45的系统,并使用它来产生一组单克隆抗体。我们在Pfs48 / 45上绘制了这些抗体的结合区域,并将它们的表位与它们的传递阻断活性相关联。最后,我们介绍了与最有效的传输阻断抗体结合的Pfs48 / 45 C端结构域的结构,并为将来的结构指导的免疫原设计提供了关键的分子信息。

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