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迈向开发有效的疟疾传播阻断疫苗。

Toward the development of effective transmission-blocking vaccines for malaria.

作者信息

Nikolaeva Daria, Draper Simon J, Biswas Sumi

机构信息

The Jenner Institute, University of Oxford, Old Road Campus Research Building, Roosevelt Drive, Headington, Oxford OX3 7DQ, UK.

出版信息

Expert Rev Vaccines. 2015 May;14(5):653-80. doi: 10.1586/14760584.2015.993383. Epub 2015 Jan 19.

Abstract

The continued global burden of malaria can in part be attributed to a complex lifecycle, with both human hosts and mosquito vectors serving as transmission reservoirs. In preclinical models of vaccine-induced immunity, antibodies to parasite sexual-stage antigens, ingested in the mosquito blood meal, can inhibit parasite survival in the insect midgut as judged by ex vivo functional studies such as the membrane feeding assay. In an era of renewed political momentum for malaria elimination and eradication campaigns, such observations have fueled support for the development and implementation of so-called transmission-blocking vaccines. While leading candidates are being evaluated using a variety of promising vaccine platforms, the field is also beginning to capitalize on global '-omics' data for the rational genome-based selection and unbiased characterization of parasite and mosquito proteins to expand the candidate list. This review covers the progress and prospects of these recent developments.

摘要

疟疾持续给全球带来负担,部分原因可归结于其复杂的生命周期,人类宿主和蚊媒均为传播宿主。在疫苗诱导免疫的临床前模型中,通过诸如膜饲法等体外功能研究判断,针对在蚊血餐中摄取的寄生虫性阶段抗原的抗体,可抑制寄生虫在昆虫中肠的存活。在消除和根除疟疾运动重新获得政治动力的时代,此类观察结果推动了对所谓传播阻断疫苗的研发和实施的支持。虽然领先的候选疫苗正在使用各种有前景的疫苗平台进行评估,但该领域也开始利用全球“组学”数据,以基于基因组的合理选择和对寄生虫和蚊媒蛋白质进行无偏表征,从而扩大候选疫苗名单。本综述涵盖了这些最新进展的情况和前景。

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