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A Plasmodium berghei sporozoite-based vaccination platform against human malaria

机译:基于伯氏疟原虫子孢子的针对人类疟疾的疫苗接种平台

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There is a pressing need for safe and highly effective Plasmodium falciparum (Pf) malaria vaccines. The circumsporozoite protein (CS), expressed on sporozoites and during early hepatic stages, is a leading target vaccine candidate, but clinical efficacy has been modest so far. Conversely, whole-sporozoite (WSp) vaccines have consistently shown high levels of sterilizing immunity and constitute a promising approach to effective immunization against malaria. Here, we describe a novel WSp malaria vaccine that employs transgenic sporozoites of rodent P. berghei (Pb) parasites as cross-species immunizing agents and as platforms for expression and delivery of PfCS (PbVac). We show that both wild-type Pb and PbVac sporozoites unabatedly infect and develop in human hepatocytes while unable to establish an infection in human red blood cells. In a rabbit model, similarly susceptible to Pb hepatic but not blood infection, we show that PbVac elicits cross-species cellular immune responses, as well as PfCS-specific antibodies that efficiently inhibit Pf sporozoite liver invasion in human hepatocytes and in mice with humanized livers. Thus, PbVac is safe and induces functional immune responses in preclinical studies, warranting clinical testing and development.
机译:迫切需要安全有效的恶性疟原虫(Pf)疟疾疫苗。在子孢子上和肝早期阶段表达的环子孢子蛋白(CS)是主要的靶疫苗候选者,但迄今为止临床疗效尚不理想。相反,全子孢子(WSp)疫苗一直显示出高水平的杀菌免疫力,构成了有效预防疟疾的有前途的方法。在这里,我们描述了一种新颖的WSp疟疾疫苗,该疫苗采用了啮齿类伯氏疟原虫(Pb)寄生虫的转基因子孢子作为跨物种免疫剂,并用作表达和传递PfCS(PbVac)的平台。我们表明,野生型Pb和PbVac子孢子都不会减弱并感染人类肝细胞,而无法在人类红细胞中建立感染。在类似地易受Pb肝感染但不受血液感染的兔模型中,我们显示PbVac会引发跨物种的细胞免疫反应,以及能有效抑制人肝细胞和人源化肝小鼠Pf子孢子肝入侵的PfCS特异性抗体。因此,PbVac是安全的,并在临床前研究中诱导功能性免疫反应,值得临床测试和开发。

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