新型减毒基孔肯雅病毒疫苗候选株在C57BL/6小鼠中引发保护性免疫。
Novel attenuated Chikungunya vaccine candidates elicit protective immunity in C57BL/6 mice.
作者信息
Hallengärd David, Kakoulidou Maria, Lulla Aleksei, Kümmerer Beate M, Johansson Daniel X, Mutso Margit, Lulla Valeria, Fazakerley John K, Roques Pierre, Le Grand Roger, Merits Andres, Liljeström Peter
机构信息
Department of Microbiology, Tumor and Cell Biology, Karolinska Institutet, Stockholm, Sweden.
出版信息
J Virol. 2014 Mar;88(5):2858-66. doi: 10.1128/JVI.03453-13. Epub 2013 Dec 26.
UNLABELLED
Chikungunya virus (CHIKV) is a reemerging mosquito-borne alphavirus that has caused severe epidemics in Africa and Asia and occasionally in Europe. As of today, there is no licensed vaccine available to prevent CHIKV infection. Here we describe the development and evaluation of novel CHIKV vaccine candidates that were attenuated by deleting a large part of the gene encoding nsP3 or the entire gene encoding 6K and were administered as viral particles or infectious genomes launched by DNA. The resulting attenuated mutants were genetically stable and elicited high magnitudes of binding and neutralizing antibodies as well as strong T cell responses after a single immunization in C57BL/6 mice. Subsequent challenge with a high dose of CHIKV demonstrated that the induced antibody responses protected the animals from viremia and joint swelling. The protective antibody response was long-lived, and a second homologous immunization further enhanced immune responses. In summary, this report demonstrates a straightforward means of constructing stable and efficient attenuated CHIKV vaccine candidates that can be administered either as viral particles or as infectious genomes launched by DNA.
IMPORTANCE
Similar to other infectious diseases, the best means of preventing CHIKV infection would be by vaccination using an attenuated vaccine platform which preferably raises protective immunity after a single immunization. However, the attenuated CHIKV vaccine candidates developed to date rely on a small number of attenuating point mutations and are at risk of being unstable or even sensitive to reversion. We report here the construction and preclinical evaluation of novel CHIKV vaccine candidates that have been attenuated by introducing large deletions. The resulting mutants proved to be genetically stable, attenuated, highly immunogenic, and able to confer durable immunity after a single immunization. Moreover, these mutants can be administered either as viral particles or as DNA-launched infectious genomes, enabling evaluation of the most feasible vaccine modality for a certain setting. These CHIKV mutants could represent stable and efficient vaccine candidates against CHIKV.
未标记
基孔肯雅病毒(CHIKV)是一种重新出现的蚊媒甲病毒,已在非洲和亚洲,偶尔也在欧洲引发严重疫情。截至目前,尚无用于预防CHIKV感染的获批疫苗。在此,我们描述了新型CHIKV候选疫苗的研发和评估,这些候选疫苗通过删除编码nsP3的大部分基因或编码6K的整个基因而减毒,并作为病毒颗粒或由DNA启动的感染性基因组进行接种。所产生的减毒突变体在基因上是稳定的,在C57BL / 6小鼠单次免疫后可引发高滴度的结合抗体和中和抗体以及强烈的T细胞反应。随后用高剂量CHIKV进行攻毒表明,诱导的抗体反应可保护动物免受病毒血症和关节肿胀。保护性抗体反应具有长效性,第二次同源免疫进一步增强了免疫反应。总之,本报告展示了一种构建稳定且高效的减毒CHIKV候选疫苗的直接方法,该疫苗可作为病毒颗粒或由DNA启动的感染性基因组进行接种。
重要性
与其他传染病类似,预防CHIKV感染的最佳方法是使用减毒疫苗平台进行接种,该平台最好在单次免疫后就能产生保护性免疫。然而,迄今为止开发的减毒CHIKV候选疫苗依赖于少数减毒点突变,存在不稳定甚至回复突变的风险。我们在此报告了通过引入大片段缺失而减毒的新型CHIKV候选疫苗的构建和临床前评估。所产生的突变体被证明在基因上是稳定的、减毒的、高度免疫原性的,并且在单次免疫后能够产生持久的免疫力。此外,这些突变体可以作为病毒颗粒或由DNA启动的感染性基因组进行接种,从而能够评估针对特定情况最可行的疫苗形式。这些CHIKV突变体可能代表了针对CHIKV的稳定且高效的候选疫苗。
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