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Malaria vaccines: identifying Plasmodium falciparum liver-stage targets

机译:疟疾疫苗:确定恶性疟原虫肝阶段目标

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摘要

The development of a highly efficacious and durable vaccine for malaria remains a top priority for global health researchers. Despite the huge rise in recognition of malaria as a global health problem and the concurrent rise in funding over the past 10–15 years, malaria continues to remain a widespread burden. The evidence of increasing resistance to anti-malarial drugs and insecticides is a growing concern. Hence, an efficacious and durable preventative vaccine for malaria is urgently needed. Vaccines are one of the most cost-effective tools and have successfully been used in the prevention and control of many diseases, however, the development of a vaccine for the Plasmodium parasite has proved difficult. Given the early success of whole sporozoite mosquito-bite delivered vaccination strategies, we know that a vaccine for malaria is an achievable goal, with sub-unit vaccines holding great promise as they are simple and cheap to both manufacture and deploy. However a major difficulty in development of sub-unit vaccines lies within choosing the appropriate antigenic target from the 5000 or so genes expressed by the parasite. Given the liver-stage of malaria represents a bottle-neck in the parasite’s life cycle, there is widespread agreement that a multi-component sub-unit malaria vaccine should preferably contain a liver-stage target. In this article we review progress in identifying and screening Plasmodium falciparum liver-stage targets for use in a malaria vaccine.
机译:研发高效耐用的疟疾疫苗仍然是全球卫生研究人员的首要任务。尽管在过去的10至15年中,人们对疟疾作为全球健康问题的认识大大增加,同时资金投入也在增加,但疟疾仍然是一个广泛的负担。对抗疟疾药物和杀虫剂的抗药性日益增强的证据日益引起人们的关注。因此,迫切需要一种有效且持久的疟疾预防疫苗。疫苗是最具成本效益的工具之一,已成功用于多种疾病的预防和控制,但是,事实证明,开发疟原虫寄生虫疫苗非常困难。鉴于整个子孢子蚊虫叮咬接种战略的早期成功,我们知道疟疾疫苗是可以实现的目标,亚单位疫苗具有很大的前景,因为它们制造和部署都简单且便宜。然而,开发亚单位疫苗的主要困难在于从寄生虫表达的5000个左右的基因中选择合适的抗原靶标。鉴于疟疾的肝阶段代表了寄生虫生命周期的瓶颈,因此人们普遍同意,多组分亚单位疟疾疫苗应优选包含肝阶段靶标。在本文中,我们回顾了鉴定和筛选用于疟疾疫苗的恶性疟原虫肝阶段靶标的进展。

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