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恶性疟原虫 7G8 挑战提供了基于 PfNF54 的 PfSPZ 疫苗在非洲疗效的保守预测。

Plasmodium falciparum 7G8 challenge provides conservative prediction of efficacy of PfNF54-based PfSPZ Vaccine in Africa.

机构信息

Institute for Genomic Sciences, University of Maryland School of Medicine, Baltimore, MD, USA.

Department of Microbiology and Immunology, University of Maryland School of Medicine, Baltimore, MD, USA.

出版信息

Nat Commun. 2022 Jun 13;13(1):3390. doi: 10.1038/s41467-022-30882-8.

Abstract

Controlled human malaria infection (CHMI) has supported Plasmodium falciparum (Pf) malaria vaccine development by providing preliminary estimates of vaccine efficacy (VE). Because CHMIs generally use Pf strains similar to vaccine strains, VE against antigenically heterogeneous Pf in the field has been required to establish VE. We increased the stringency of CHMI by selecting a Brazilian isolate, Pf7G8, which is genetically distant from the West African parasite (PfNF54) in our PfSPZ vaccines. Using two regimens to identically immunize US and Malian adults, VE over 24 weeks in the field was as good as or better than VE against CHMI at 24 weeks in the US. To explain this finding, here we quantify differences in the genome, proteome, and predicted CD8 T cell epitopes of PfNF54 relative to 704 Pf isolates from Africa and Pf7G8. We show that Pf7G8 is more distant from PfNF54 than any African isolates tested. We propose VE against Pf7G8 CHMI for providing pivotal data for malaria vaccine licensure for travelers to Africa, and potentially for endemic populations, because the genetic distance of Pf7G8 from the Pf vaccine strain makes it a stringent surrogate for Pf parasites in Africa.

摘要

人体疟疾感染控制(CHMI)通过提供疫苗效力(VE)的初步估计,支持恶性疟原虫(Pf)疟疾疫苗的开发。由于 CHMI 通常使用与疫苗株相似的 Pf 株,因此需要对现场具有抗原异质性的 Pf 进行 VE 评估,以确定 VE。我们通过选择巴西分离株 Pf7G8 来增加 CHMI 的严格性,该分离株在遗传上与我们 PfSPZ 疫苗中的西非寄生虫(PfNF54)相距甚远。使用两种方案对美国和马里成年人进行相同的免疫,在现场的 24 周 VE 与美国 CHMI 的 24 周 VE 一样好或更好。为了解释这一发现,我们在这里量化了 PfNF54 与来自非洲和 Pf7G8 的 704 个 Pf 分离株的基因组、蛋白质组和预测的 CD8 T 细胞表位之间的差异。我们表明,Pf7G8 与 PfNF54 的距离比任何非洲分离株都远。我们建议使用 Pf7G8 CHMI 的 VE,为前往非洲的旅行者和潜在的流行地区人群提供疟疾疫苗许可的关键数据,因为 Pf7G8 与 Pf 疫苗株的遗传距离使其成为非洲 Pf 寄生虫的严格替代物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/19cf/9192756/9d9845591374/41467_2022_30882_Fig1_HTML.jpg

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