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福尔马林灭活全病毒和重组亚单位黄病毒疫苗。

Formalin-inactivated whole virus and recombinant subunit flavivirus vaccines.

作者信息

Eckels Kenneth H, Putnak Robert

机构信息

Division of Communicable Diseases and Immunology, Walter Reed Army Institute of Research, Silver Spring, Maryland 20910, USA.

出版信息

Adv Virus Res. 2003;61:395-418. doi: 10.1016/s0065-3527(03)61010-9.

Abstract

The Flaviviridae is a family of arthropod-borne, enveloped, RNA viruses that contain important human pathogens such as yellow fever (YF), Japanese encephalitis (JE), tick-borne encephalitis (TBE), West Nile (WN), and the dengue (DEN) viruses. Vaccination is the most effective means of disease prevention for these viral infections. A live-attenuated vaccine for YF, and inactivated vaccines for JE and TBE have significantly reduced the incidence of disease for these viruses, while licensed vaccines for DEN and WN are still lacking despite a significant disease burden associated with these infections. This review focuses on inactivated and recombinant subunit vaccines (non-replicating protein vaccines) in various stages of laboratory development and human testing. A purified, inactivated vaccine (PIV) candidate for DEN will soon be evaluated in a phase 1 clinical trial, and a second-generation JE PIV produced using similar technology has advanced to phase 2/3 trials. The inactivated TBE vaccine used successfully in Europe for almost 30 years continues to be improved by additional purification, new stabilizers, an adjuvant, and better immunization schedules. The recent development of an inactivated WN vaccine for domestic animals demonstrates the possibility of producing a similar vaccine for human use. Advances in flavivirus gene expression technology have led to the production of several recombinant subunit antigen vaccine candidates in a variety of expression systems. Some of these vaccines have shown sufficient promise in animal models to be considered as candidates for evaluation in clinical trials. Feasibility of non-replicating flavivirus vaccines has been clearly demonstrated and further development is now warranted.

摘要

黄病毒科是一类节肢动物传播的包膜RNA病毒,其中包含重要的人类病原体,如黄热病(YF)、日本脑炎(JE)、蜱传脑炎(TBE)、西尼罗河病毒(WN)和登革热(DEN)病毒。疫苗接种是预防这些病毒感染的最有效手段。黄热病的减毒活疫苗以及日本脑炎和蜱传脑炎的灭活疫苗已显著降低了这些病毒导致的疾病发病率,而尽管登革热和西尼罗河病毒感染带来了巨大的疾病负担,但针对它们的许可疫苗仍然缺乏。本综述重点关注处于实验室研发和人体试验不同阶段的灭活疫苗和重组亚单位疫苗(非复制性蛋白疫苗)。一种纯化的登革热灭活疫苗(PIV)候选疫苗即将进入1期临床试验,采用类似技术生产的第二代日本脑炎PIV已进入2/3期试验。在欧洲成功使用了近30年的灭活蜱传脑炎疫苗,通过进一步纯化、新型稳定剂、佐剂和更好的免疫接种方案不断改进。最近一种用于家畜的西尼罗河病毒灭活疫苗的研发表明,有可能生产出供人类使用的类似疫苗。黄病毒基因表达技术的进展已导致在多种表达系统中生产出几种重组亚单位抗原疫苗候选物。其中一些疫苗在动物模型中已显示出足够的前景,可被视为临床试验评估的候选疫苗。非复制性黄病毒疫苗的可行性已得到明确证明,现在有必要进一步研发。

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