首页> 外文期刊>Malaria Journal >Yeast lysates carrying the nucleoprotein from measles virus vaccine as a novel subunit vaccine platform to deliver Plasmodium circumsporozoite antigen
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Yeast lysates carrying the nucleoprotein from measles virus vaccine as a novel subunit vaccine platform to deliver Plasmodium circumsporozoite antigen

机译:携带来自麻疹病毒疫苗的核蛋白的酵母裂解物,作为一种新的亚单位疫苗平台,可提供疟原虫环子孢子抗原

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BackgroundYeast cells represent an established bioreactor to produce recombinant proteins for subunit vaccine development. In addition, delivery of vaccine antigens directly within heat-inactivated yeast cells is attractive due to the adjuvancy provided by the yeast cell. In this study, Pichia pastoris yeast lysates carrying the nucleoprotein (N) from the measles vaccine virus were evaluated as a novel subunit vaccine platform to deliver the circumsporozoite surface antigen (CS) of Plasmodium . When expressed in Pichia pastoris yeast, the N protein auto-assembles into highly multimeric ribonucleoparticles (RNPs). The CS antigen from Plasmodium berghei (PbCS) was expressed in Pichia pastoris yeast in fusion with N, generating recombinant PbCS-carrying RNPs in the cytoplasm of yeast cells. ResultsWhen evaluated in mice after 3–5?weekly subcutaneous injections, yeast lysates containing N-PbCS RNPs elicited strong anti-PbCS humoral responses, which were PbCS-dose dependent and reached a plateau by the pre-challenge time point. Protective efficacy of yeast lysates was dose-dependent, although anti-PbCS antibody titers were not predictive of protection. Multimerization of PbCS on RNPs was essential for providing benefit against infection, as immunization with monomeric PbCS delivered in yeast lysates was not protective. Three weekly injections with N-PbCS yeast lysates in combination with alum adjuvant produced sterile protection in two out of six mice, and significantly reduced parasitaemia in the other individuals from the same group. This parasitaemia decrease was of the same extent as in mice immunized with non-adjuvanted N-PbCS yeast lysates, providing evidence that the yeast lysate formulation did not require accessory adjuvants for eliciting efficient parasitaemia reduction. ConclusionsThis study demonstrates that yeast lysates are an attractive auto-adjuvant and efficient platform for delivering multimeric PbCS on measles N-based RNPs. By combining yeast lysates that carry RNPs with a large panel of Plasmodium antigens, this technology could be applied to developing a multivalent vaccine against malaria.
机译:背景酵母细胞代表了一种成熟的生物反应器,可产生用于亚单位疫苗开发的重组蛋白。另外,由于酵母细胞提供的辅助作用,直接在热灭活的酵母细胞内递送疫苗抗原是有吸引力的。在这项研究中,带有麻疹疫苗病毒核蛋白(N)的巴斯德毕赤酵母酵母裂解物被评估为一种新的亚单位疫苗平台,可用于传播疟原虫的环子孢子表面抗原(CS)。当在巴斯德毕赤酵母中表达时,N蛋白会自动组装成高度多聚的核糖核酸颗粒(RNP)。伯氏疟原虫(PbCS)的CS抗原在巴斯德毕赤酵母酵母中与N融合表达,在酵母细胞质中产生携带PbCS的重组RNP。结果当在每周皮下注射3-5次后对小鼠进行评估时,含有N-PbCS RNPs的酵母裂解物会引起强烈的抗PbCS体液反应,这是PbCS剂量依赖性的,并且在攻击前的时间点达到平稳。酵母裂解物的保护功效是剂量依赖性的,尽管抗PbCS抗体滴度不能预测保护作用。 PbCS在RNP上的多聚化对于提供抗感染作用至关重要,因为用酵母裂解液中的单体PbCS进行免疫接种没有保护性。每周三次注射N-PbCS酵母裂解物和明矾佐剂,在六分之二的小鼠中产生了无菌保护,并显着降低了同一组其他个体的寄生虫血症。这种寄生虫血症的减少程度与用未佐剂的N-PbCS酵母裂解物免疫的小鼠相同,提供了证据表明酵母裂解物制剂不需要辅助佐剂即可有效地降低寄生虫血症。结论这项研究表明酵母裂解物是在基于麻疹N的RNPs上递送多聚体PbCS的有吸引力的自动佐剂和高效平台。通过将携带RNP的酵母裂解物与大量疟原虫抗原结合,该技术可用于开发抗疟疾的多价疫苗。

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