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RTS,S/AS01疟疾疫苗的保护性抗体阈值与小鼠模型中的抗原和佐剂剂量相关。

Protective antibody threshold of RTS,S/AS01 malaria vaccine correlates antigen and adjuvant dose in mouse model.

作者信息

Genito Christopher J, Brooks Katherine, Smith Alexis, Ryan Emma, Soto Kim, Li Yuanzhang, Warter Lucile, Dutta Sheetij

机构信息

Structural Vaccinology Laboratory, Biologics Research and Development Branch, Walter Reed Army Institute of Research, Silver Spring, MD, 20910, USA.

Center for Enabling Capabilities, Walter Reed Army Institute of Research, Silver Spring, MD, 20910, USA.

出版信息

NPJ Vaccines. 2023 Aug 10;8(1):114. doi: 10.1038/s41541-023-00714-x.

Abstract

Mouse models are useful for the early down-selection of malaria vaccine candidates. The Walter Reed Army Institute of Research has optimized a transgenic Plasmodium berghei sporozoite challenge model to compare the efficacy of Plasmodium falciparum circumsporozoite protein (CSP) vaccines. GSK's RTS,S vaccine formulated in the adjuvant AS01 can protect malaria-naïve individuals against malaria. We report that the RTS,S/AS01 vaccine induces high level sterile protection in our mouse model. Down titration of the antigen at a constant AS01 dose revealed a potent antigen dose-sparing effect and the superiority of RTS,S/AS01 over a soluble CSP antigen. RTS,S-mediated protective immunity was associated with a threshold of major repeat antibody titer. Combined titration of the antigen and adjuvant showed that reducing the adjuvant could improve antibody boosting post-3rd vaccination and reduce the threshold antibody concentration required for protection. Mouse models can provide a pathway for preclinical assessment of strategies to improve CSP vaccines against malaria.

摘要

小鼠模型有助于早期筛选疟疾疫苗候选物。沃尔特·里德陆军研究所优化了一种转基因伯氏疟原虫子孢子攻击模型,以比较恶性疟原虫环子孢子蛋白(CSP)疫苗的疗效。葛兰素史克公司在佐剂AS01中配制的RTS,S疫苗可保护未感染疟疾的个体免受疟疾侵害。我们报告称,RTS,S/AS01疫苗在我们的小鼠模型中诱导了高水平的无菌保护。在AS01剂量恒定的情况下对抗原进行滴定,结果显示出强大的抗原剂量节省效应以及RTS,S/AS01相对于可溶性CSP抗原的优越性。RTS,S介导的保护性免疫与主要重复抗体滴度的阈值相关。对抗原和佐剂进行联合滴定表明,减少佐剂可改善第三次疫苗接种后的抗体增强效果,并降低保护所需的阈值抗体浓度。小鼠模型可为改进抗疟疾CSP疫苗策略的临床前评估提供一条途径。

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