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病毒样颗粒疫苗在丝状病毒中的研究进展。

Advances in virus-like particle vaccines for filoviruses.

机构信息

Vaccine Development, Integrated Biotherapeutics, 21 Firstfield Rd, Ste 100, Gaithersburg, MD 20878, USA.

出版信息

J Infect Dis. 2011 Nov;204 Suppl 3(Suppl 3):S1053-9. doi: 10.1093/infdis/jir346.

DOI:10.1093/infdis/jir346
PMID:21987741
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3189993/
Abstract

Ebola virus (EBOV) and Marburg virus (MARV) are among the deadliest human pathogens, with no vaccines or therapeutics available. Multiple vaccine platforms have been tested for efficacy as prophylactic pretreatments or therapeutics for prevention of filovirus hemorrhagic fever. Most successful vaccines are based on a virus-vectored approach expressing the protective glycoprotein (GP); protein-based subunit and DNA vaccines have been tested with moderate success. Virus-like particle (VLP) vaccines have realized promising results when tested in both rodents and nonhuman primates. VLPs rely on the natural properties of the viral matrix protein (VP) 40 to drive budding of filamentous particles that can also incorporate ≥ 1 other filovirus protein, including GP, VP24, and nucleoprotein (NP). Filovirus VLP vaccines have used particles containing 2 or 3 (GP and VP40, with or without NP) viral proteins generated in either mammalian or insect cells. Early studies successfully demonstrated efficacy of bivalent VLP vaccines in rodents; more recent studies have shown the ability of the VLP vaccines containing GP, NP, and VP40 to confer complete homologous protection against Ebola virus and Marburg virus in a prophylactic setting against in macaques. This review will discuss published work to date regarding development of the VLP vaccines for prevention of lethal filovirus hemorrhagic fever.

摘要

埃博拉病毒 (EBOV) 和马尔堡病毒 (MARV) 是最致命的人类病原体之一,目前尚无可用的疫苗或疗法。已经测试了多种疫苗平台,以评估其作为预防丝状病毒出血热的预防性预处理或治疗的功效。大多数成功的疫苗都基于病毒载体方法,表达保护性糖蛋白 (GP);已经测试了基于蛋白质的亚单位和 DNA 疫苗,但取得了中等成功。病毒样颗粒 (VLP) 疫苗在啮齿动物和非人类灵长类动物中的测试中取得了有希望的结果。VLP 依赖病毒基质蛋白 (VP) 40 的天然特性来驱动丝状颗粒的出芽,这些颗粒还可以包含≥1 种其他丝状病毒蛋白,包括 GP、VP24 和核蛋白 (NP)。丝状病毒 VLP 疫苗使用在哺乳动物或昆虫细胞中生成的含有 2 种或 3 种(GP 和 VP40,有或没有 NP)病毒蛋白的颗粒。早期研究成功地证明了二价 VLP 疫苗在啮齿动物中的功效;最近的研究表明,含有 GP、NP 和 VP40 的 VLP 疫苗能够在预防猕猴中预防同源致死性埃博拉病毒和马尔堡病毒方面提供完全同源保护。这篇综述将讨论迄今为止关于 VLP 疫苗开发用于预防致命丝状病毒出血热的已发表工作。

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Oligomerization of Ebola virus VP40 is essential for particle morphogenesis and regulation of viral transcription.埃博拉病毒 VP40 的寡聚化对于病毒粒子形态发生和病毒转录的调节是必需的。
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Viral strategies for the evasion of immunogenic cell death.病毒逃避免疫原性细胞死亡的策略。
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Virus-like particles as particulate vaccines.作为颗粒疫苗的病毒样颗粒
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Marburg virus evades interferon responses by a mechanism distinct from ebola virus.马尔堡病毒通过一种与埃博拉病毒不同的机制逃避干扰素反应。
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Conserved motifs within Ebola and Marburg virus VP40 proteins are important for stability, localization, and subsequent budding of virus-like particles.埃博拉病毒和马尔堡病毒 VP40 蛋白内的保守基序对于病毒样颗粒的稳定性、定位和随后的出芽是重要的。
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Protection against lethal challenge by Ebola virus-like particles produced in insect cells.昆虫细胞中产生的埃博拉病毒样颗粒对致死性攻击的保护作用。
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Monovalent virus-like particle vaccine protects guinea pigs and nonhuman primates against infection with multiple Marburg viruses.单价病毒样颗粒疫苗可保护豚鼠和非人类灵长类动物免受多种马尔堡病毒感染。
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