首页> 美国卫生研究院文献>Journal of Virology >Replication and Clearance of Venezuelan Equine Encephalitis Virus from the Brains of Animals Vaccinated with Chimeric SIN/VEE Viruses
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Replication and Clearance of Venezuelan Equine Encephalitis Virus from the Brains of Animals Vaccinated with Chimeric SIN/VEE Viruses

机译:从接种嵌合SIN / VEE病毒的动物的脑中复制和清除委内瑞拉马脑炎病毒

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摘要

Venezuelan equine encephalitis virus (VEEV) is an important, naturally emerging zoonotic pathogen. Recent outbreaks in Venezuela and Colombia in 1995, involving an estimated 100,000 human cases, indicate that VEEV still poses a serious public health threat. To develop a safe, efficient vaccine that protects against disease resulting from VEEV infection, we generated chimeric Sindbis (SIN) viruses expressing structural proteins of different strains of VEEV and analyzed their replication in vitro and in vivo, as well as the characteristics of the induced immune responses. None of the chimeric SIN/VEE viruses caused any detectable disease in adult mice after either intracerebral (i.c.) or subcutaneous (s.c.) inoculation, and all chimeras were more attenuated than the vaccine strain, VEEV TC83, in 6-day-old mice after i.c. infection. All vaccinated mice were protected against lethal encephalitis following i.c., s.c., or intranasal (i.n.) challenge with the virulent VEEV ZPC738 strain (ZPC738). In spite of the absence of clinical encephalitis in vaccinated mice challenged with ZPC738 via i.n. or i.c. route, we regularly detected high levels of infectious challenge virus in the central nervous system (CNS). However, infectious virus was undetectable in the brains of all immunized animals at 28 days after challenge. Hamsters vaccinated with chimeric SIN/VEE viruses were also protected against s.c. challenge with ZPC738. Taken together, our findings suggest that these chimeric SIN/VEE viruses are safe and efficacious in adult mice and hamsters and are potentially useful as VEEV vaccines. In addition, immunized animals provide a useful model for studying the mechanisms of the anti-VEEV neuroinflammatory response, leading to the reduction of viral titers in the CNS and survival of animals.
机译:委内瑞拉马脑炎病毒(VEEV)是一种重要的自然产生的人畜共患病原体。 1995年委内瑞拉和哥伦比亚的最近暴发,估计有100,000例人类病例,这表明VEEV仍然构成严重的公共卫生威胁。为了开发一种安全,有效的疫苗来预防VEEV感染引起的疾病,我们产生了表达SVE的嵌合Sindbis(SIN)病毒,它们表达不同VEEV株的结构蛋白,并分析了它们在体内和体外的复制以及诱导的特征。免疫反应。在脑内(ic)或皮下(sc)接种后,没有嵌合SIN / VEE病毒在成年小鼠中引起任何可检测到的疾病,并且在接种后6天的小鼠中,所有嵌合体均比疫苗株VEEV TC83更弱。我知道了感染。在强毒VEEV ZPC738株(s.c.)或鼻内(i.n.)攻击后,所有接种疫苗的小鼠均受到保护,免受致命性脑炎的侵害。尽管不存在临床脑炎,但在经i.n.或路线中,我们定期在中枢神经系统(CNS)中检测到高水平的传染性挑战病毒。然而,在攻击后28天,在所有免疫动物的大脑中均未检测到传染性病毒。接种了SIN / VEE嵌合病毒的仓鼠也受到保护,免受s.c.侵害。 ZPC738挑战。综上所述,我们的发现表明,这些嵌合SIN / VEE病毒在成年小鼠和仓鼠中是安全有效的,并且有可能作为VEEV疫苗使用。另外,经免疫的动物为研究抗VEEV神经炎症反应的机制提供了有用的模型,该机制导致CNS中病毒滴度的降低和动物的存活。

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