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新型 DNA 启动的委内瑞拉马脑炎病毒疫苗,具有重排的基因组。

Novel DNA-launched Venezuelan equine encephalitis virus vaccine with rearranged genome.

机构信息

Medigen, Inc., 8420 Gas House Pike, Suite S, Frederick, MD 21701, USA.

University of Louisville, 505 S Hancock St., Louisville, KY 40202, USA.

出版信息

Vaccine. 2019 May 31;37(25):3317-3325. doi: 10.1016/j.vaccine.2019.04.072. Epub 2019 May 6.

Abstract

Novel live-attenuated V4020 vaccine was prepared for Venezuelan equine encephalitis virus (VEEV), an alphavirus from the Togaviridae family. The genome of V4020 virus was rearranged, with the capsid gene expressed using a duplicate subgenomic promoter downstream from the glycoprotein genes. V4020 also included both attenuating mutations from the TC83 VEEV vaccine secured by mutagenesis to prevent reversion mutations. The full-length infectious RNA of V4020 vaccine virus was expressed from pMG4020 plasmid downstream from the CMV promoter and launched replication of live-attenuated V4020 in vitro or in vivo. BALB/c mice vaccinated with a single dose of V4020 virus or with pMG4020 plasmid had no adverse reactions to vaccinations and developed high titers of neutralizing antibodies. After challenge with the wild type VEEV, vaccinated mice survived with no morbidity, while all unvaccinated controls succumbed to lethal infection. Intracranial injections in mice showed attenuated replication of V4020 vaccine virus as compared to the TC83. We conclude that V4020 vaccine has safety advantage over TC83, while provides equivalent protection in a mouse VEEV challenge model.

摘要

新型活减毒 V4020 疫苗被制备用于委内瑞拉马脑炎病毒(VEEV),这是一种来自披膜病毒科的甲病毒。V4020 病毒的基因组发生了重排,衣壳蛋白基因使用来自糖蛋白基因下游的重复亚基因组启动子进行表达。V4020 还包括通过诱变获得的来自 TC83 VEEV 疫苗的两种减毒突变,以防止回复突变。V4020 疫苗病毒全长感染性 RNA 由 pMG4020 质粒表达,该质粒位于 CMV 启动子的下游,并在体外或体内启动活减毒 V4020 的复制。单次接种 V4020 病毒或 pMG4020 质粒的 BALB/c 小鼠对疫苗接种没有不良反应,并产生了高滴度的中和抗体。用野生型 VEEV 攻毒后,接种疫苗的小鼠无发病率存活,而所有未接种疫苗的对照小鼠均死于致死性感染。与 TC83 相比,V4020 疫苗在小鼠颅内注射中显示出减毒复制。我们得出结论,V4020 疫苗在安全性方面优于 TC83,同时在小鼠 VEEV 攻毒模型中提供等效保护。

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