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初步鉴定间日疟原虫(Plasmodium vivax)子孢子抗原作为红细胞前期候选疫苗。

Preliminary characterization of Plasmodium vivax sporozoite antigens as pre-erythrocytic vaccine candidates.

机构信息

Center for Global Health and Interdisciplinary Research, College of Public Health, University of South Florida, Tampa, Florida, United States of America.

Department of Molecular Medicine, Morsani College of Medicine, University of South Florida, Tampa, Florida, United States of America.

出版信息

PLoS Negl Trop Dis. 2023 Sep 13;17(9):e0011598. doi: 10.1371/journal.pntd.0011598. eCollection 2023 Sep.

Abstract

Plasmodium vivax pre-erythrocytic (PE) vaccine research has lagged far behind efforts to develop Plasmodium falciparum vaccines. There is a critical gap in our knowledge of PE antigen targets that can induce functionally inhibitory neutralizing antibody responses. To overcome this gap and guide the selection of potential PE vaccine candidates, we considered key characteristics such as surface exposure, essentiality to infectivity and liver stage development, expression as recombinant proteins, and functional immunogenicity. Selected P. vivax sporozoite antigens were surface sporozoite protein 3 (SSP3), sporozoite microneme protein essential for cell traversal (SPECT1), sporozoite surface protein essential for liver-stage development (SPELD), and M2 domain of MAEBL. Sequence analysis revealed little variation occurred in putative B-cell and T-cell epitopes of the PE candidates. Each antigen was tested for expression as refolded recombinant proteins using an established bacterial expression platform and only SPELD failed. The successfully expressed antigens were immunogenic in vaccinated laboratory mice and were positively reactive with serum antibodies of P. vivax-exposed residents living in an endemic region in Thailand. Vaccine immune antisera were tested for reactivity to native sporozoite proteins and for their potential vaccine efficacy using an in vitro inhibition of liver stage development assay in primary human hepatocytes quantified on day 6 post-infection by high content imaging analysis. The anti-PE sera produced significant inhibition of P. vivax sporozoite invasion and liver stage development. This report provides an initial characterization of potential new PE candidates for a future P. vivax vaccine.

摘要

间日疟原虫(Plasmodium vivax)红细胞前期(PE)疫苗的研究远远落后于恶性疟原虫(Plasmodium falciparum)疫苗的研发。我们对能够诱导具有功能抑制性中和抗体反应的 PE 抗原靶标知之甚少,存在着巨大的知识空白。为了克服这一空白并指导潜在 PE 疫苗候选物的选择,我们考虑了关键特征,如表面暴露、对感染性和肝期发育的必要性、作为重组蛋白的表达以及功能免疫原性。选择的间日疟原虫子孢子抗原包括表面子孢子蛋白 3(SSP3)、对细胞穿入至关重要的子孢子微线蛋白 1(SPECT1)、对肝期发育至关重要的子孢子表面蛋白(SPELD)和 MAEBL 的 M2 结构域。序列分析显示 PE 候选物的潜在 B 细胞和 T 细胞表位几乎没有变异。使用已建立的细菌表达平台测试了每个抗原作为重折叠重组蛋白的表达,只有 SPELD 失败。成功表达的抗原在接种的实验小鼠中具有免疫原性,并与生活在泰国流行地区的间日疟原虫暴露居民的血清抗体呈阳性反应。疫苗免疫血清被测试与天然子孢子蛋白的反应性及其在体外用人原代肝细胞进行的肝期发育抑制测定中的潜在疫苗功效,在感染后第 6 天通过高内涵成像分析进行量化。抗 PE 血清对子孢子的入侵和肝期发育具有显著的抑制作用。本报告初步描述了未来间日疟原虫疫苗的潜在新的 PE 候选物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/82c3/10519608/d92db7fd51bc/pntd.0011598.g001.jpg

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