首页> 美国卫生研究院文献>The Journal of Clinical Investigation >Pfs230 yields higher malaria transmission–blocking vaccine activity than Pfs25 in humans but not mice
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Pfs230 yields higher malaria transmission–blocking vaccine activity than Pfs25 in humans but not mice

机译:PFS230产生比人类的PFS25更高的疟疾传播疫苗活性但不是小鼠

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摘要

Vaccines that block human-to-mosquito Plasmodium transmission are needed for malaria eradication, and clinical trials have targeted zygote antigen Pfs25 for decades. We reported that a Pfs25 protein-protein conjugate vaccine formulated in alum adjuvant induced serum functional activity in both US and Malian adults. However, antibody levels declined rapidly, and transmission-reducing activity required 4 vaccine doses. Functional immunogenicity and durability must be improved before advancing transmission-blocking vaccines further in clinical development. We hypothesized that the prefertilization protein Pfs230 alone or in combination with Pfs25 would improve functional activity.
机译:为疟疾根除需要阻止人对蚊虫疟原虫传播的疫苗,临床试验已经瞄准了抗原抗原PFS25几十年。我们报道,在美国和麦丽兰成人中,在Alum佐剂诱导的血清功能活性中配制的PFS25蛋白 - 蛋白缀合物疫苗。然而,抗体水平迅速下降,并且需要4种疫苗剂量的传递减少活性。在临床开发中进一步推进传播疫苗之前,必须改善功能性免疫原性和耐久性。我们假设单独或与PFS25组合的偏好蛋白质PFS230将改善功能活性。

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