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用于疫苗开发的小鼠感染模型:以疟疾为例。

Murine infection models for vaccine development: the malaria example.

作者信息

Matuschewski Kai

机构信息

Parasitology Unit; Max Planck Institute for Infection Biology; Berlin, Germany; Institute of Biology; Humboldt University; Berlin, Germany.

出版信息

Hum Vaccin Immunother. 2013 Mar;9(3):450-6. doi: 10.4161/hv.23218. Epub 2012 Dec 18.

Abstract

Vaccines are developed and eventually licensed following consecutive human clinical trials. Malaria is a potential fatal vector-borne infectious disease caused by blood infection of the single-cell eukaryote Plasmodium. Pathogen stage conversion is a hallmark of parasites in general and permits unprecedented vaccine strategies. In the case of malaria, experimental human challenge infections with Plasmodium falciparum sporozoites can be performed under rigorous clinical supervision. This rare opportunity in vaccinology has permitted many small-scale phase II anti-malaria vaccine studies using experimental homologous challenge infections. Demonstration of safety and lasting sterile protection are central endpoints to advance a candidate malaria vaccine approach to phase II field trials. A growing list of antigens as targets for subunit development makes pre-selection and prioritization of vaccine candidates in murine infection models increasingly important. Preclinical assessment in challenge studies with murine Plasmodium species also led to the development of whole organism vaccine approaches. They include live attenuated, metabolically active parasites that educate effector memory T cells to recognize and inactivate developing parasites inside host cells. Here, opportunities from integrating challenge experiments with murine Plasmodium parasites into malaria vaccine development will be discussed.

摘要

疫苗是经过连续的人体临床试验后研发并最终获得许可的。疟疾是一种由单细胞真核生物疟原虫血液感染引起的潜在致命性媒介传播传染病。病原体阶段转换是寄生虫的一个普遍特征,这使得前所未有的疫苗策略成为可能。就疟疾而言,可以在严格的临床监督下进行用恶性疟原虫子孢子对人体进行的实验性感染挑战。疫苗学中的这个难得机会使得许多小规模的II期抗疟疾疫苗研究能够利用实验性同源感染挑战来开展。证明安全性和持久的无菌保护是将候选疟疾疫苗方法推进到II期现场试验的核心终点。作为亚单位开发靶点的抗原越来越多,这使得在小鼠感染模型中对候选疫苗进行预选和排序变得越来越重要。用鼠疟原虫物种进行的感染挑战研究中的临床前评估也促成了全生物体疫苗方法的发展。它们包括减毒活的、代谢活跃的寄生虫,这些寄生虫能训练效应记忆T细胞识别并灭活宿主细胞内正在发育的寄生虫。在此,将讨论把用鼠疟原虫进行的感染挑战实验整合到疟疾疫苗研发中的机会。

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