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一种植物生产的基于Pvs25的间日疟原虫亚单位疫苗的传播阻断效力和免疫原性。

Transmission blocking potency and immunogenicity of a plant-produced Pvs25-based subunit vaccine against Plasmodium vivax.

作者信息

Blagborough A M, Musiychuk K, Bi H, Jones R M, Chichester J A, Streatfield S, Sala K A, Zakutansky S E, Upton L M, Sinden R E, Brian I, Biswas S, Sattabonkot J, Yusibov V

机构信息

Department of Life Sciences, Sir Alexander Fleming Building, Imperial College London, Imperial College Road, South Kensington, London SW7 2AZ, UK.

Fraunhofer USA Center for Molecular Biotechnology, Newark, DE, USA.

出版信息

Vaccine. 2016 Jun 14;34(28):3252-9. doi: 10.1016/j.vaccine.2016.05.007. Epub 2016 May 10.

Abstract

Malaria transmission blocking (TB) vaccines (TBVs) directed against proteins expressed on the sexual stages of Plasmodium parasites are a potentially effective means to reduce transmission. Antibodies induced by TBVs block parasite development in the mosquito, and thus inhibit transmission to further human hosts. The ookinete surface protein P25 is a primary target for TBV development. Recently, transient expression in plants using hybrid viral vectors has demonstrated potential as a strategy for cost-effective and scalable production of recombinant vaccines. Using a plant virus-based expression system, we produced recombinant P25 protein of Plasmodium vivax (Pvs25) in Nicotiana benthamiana fused to a modified lichenase carrier protein. This candidate vaccine, Pvs25-FhCMB, was purified, characterized and evaluated for immunogenicity and efficacy using multiple adjuvants in a transgenic rodent model. An in vivo TB effect of up to a 65% reduction in intensity and 54% reduction in prevalence was observed using Abisco-100 adjuvant. The ability of this immunogen to induce a TB response was additionally combined with heterologous prime-boost vaccination with viral vectors expressing Pvs25. Significant blockade was observed when combining both platforms, achieving a 74% and 68% reduction in intensity and prevalence, respectively. This observation was confirmed by direct membrane feeding on field P. vivax samples, resulting in reductions in intensity/prevalence of 85.3% and 25.5%. These data demonstrate the potential of this vaccine candidate and support the feasibility of expressing Plasmodium antigens in a plant-based system for the production of TBVs, while demonstrating the potential advantages of combining multiple vaccine delivery systems to maximize efficacy.

摘要

针对疟原虫有性阶段表达的蛋白质的疟疾传播阻断(TB)疫苗是减少传播的一种潜在有效手段。TB疫苗诱导产生的抗体可阻断寄生虫在蚊子体内的发育,从而抑制向更多人类宿主的传播。动合子表面蛋白P25是TB疫苗开发的主要靶点。最近,利用杂交病毒载体在植物中瞬时表达已显示出作为一种具有成本效益且可扩展的重组疫苗生产策略的潜力。我们使用基于植物病毒的表达系统,在本氏烟草中生产了与修饰的地衣酶载体蛋白融合的间日疟原虫重组P25蛋白(Pvs25)。这种候选疫苗Pvs25-FhCMB经过纯化、表征,并在转基因啮齿动物模型中使用多种佐剂评估了其免疫原性和效力。使用Abisco-100佐剂观察到体内TB效应,强度降低高达65%,流行率降低54%。这种免疫原诱导TB反应的能力还与用表达Pvs25的病毒载体进行异源初免-加强疫苗接种相结合。当两种平台联合使用时观察到显著的阻断效果,强度和流行率分别降低了74%和68%。通过对野外间日疟原虫样本直接进行膜饲法证实了这一观察结果,强度/流行率分别降低了85.3%和25.5%。这些数据证明了这种候选疫苗的潜力,并支持在基于植物的系统中表达疟原虫抗原以生产TB疫苗的可行性,同时证明了联合多种疫苗递送系统以最大化效力的潜在优势。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2e2f/4915602/d13747d934c1/gr1.jpg

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