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减毒活疫苗日本脑炎疫苗 SA14 - 14 - 2 株与其减毒前的强毒株亲本 SA14 株的比较:体内外异同

Comparison of the live-attenuated Japanese encephalitis vaccine SA14-14-2 strain with its pre-attenuated virulent parent SA14 strain: similarities and differences in vitro and in vivo.

作者信息

Yun Sang-Im, Song Byung-Hak, Polejaeva Irina A, Davies Christopher J, White Kenneth L, Lee Young-Min

机构信息

Department of Animal, Dairy, and Veterinary Sciences, Utah Science Technology and Research, College of Agriculture and Applied Sciences, Utah State University, 4815 Old Main Hill, Logan, UT 84322, USA.

出版信息

J Gen Virol. 2016 Oct;97(10):2575-2591. doi: 10.1099/jgv.0.000574. Epub 2016 Aug 5.

Abstract

Japanese encephalitis virus (JEV) is the main cause of acute viral encephalitis, primarily affecting children and young adults in the Asia-Pacific region. JEV is a vaccine-preventable pathogen, with four types of JE vaccine licensed in different regions of the world. To date, the most common JEV strain used in vaccine development and production is SA14-14-2, an attenuated strain derived from its wild-type parental strain SA14. In this study, we directly compared the phenotypic and genotypic characteristics of SA14 and SA14-14-2 to determine the biological and genetic properties associated with their differential virulence. In susceptible BHK-21 cells, SA14-14-2 grew slightly more slowly and formed smaller plaques than SA14, but unlike SA14, it showed almost no expression of the viral protein NS1', the product of a conserved predicted RNA pseudoknot-mediated ribosomal frameshift. In weanling ICR mice, SA14-14-2 was highly attenuated in terms of both neuroinvasiveness and neurovirulence, with its median lethal doses invariably over five logs higher than those of SA14 when inoculated intramuscularly and intracerebrally. Interestingly, the neurovirulence of SA14-14-2 was dependent on mouse age, with the 1- to 7-day-old mice being highly susceptible and the 14- to 21-day-old mice becoming resistant to intracerebral inoculation. At the genome level, SA14-14-2 differed from SA14 by 57 nucleotides, including one silent G-to-A substitution at position 3599 within the predicted RNA pseudoknot for NS1' synthesis; of the 57 differences, 25 resulted in amino acid substitutions. Our data pave the way for the development of new genetically modified JE vaccines.

摘要

日本脑炎病毒(JEV)是急性病毒性脑炎的主要病因,主要影响亚太地区的儿童和年轻人。JEV是一种可通过疫苗预防的病原体,世界不同地区有四种类型的乙脑疫苗获得许可。迄今为止,疫苗研发和生产中最常用的JEV毒株是SA14-14-2,它是一种从野生型亲本毒株SA14衍生而来的减毒株。在本研究中,我们直接比较了SA14和SA14-14-2的表型和基因型特征,以确定与其不同毒力相关的生物学和遗传特性。在易感的BHK-21细胞中,SA14-14-2的生长速度比SA14略慢,形成的蚀斑也比SA14小,但与SA14不同的是,它几乎不表达病毒蛋白NS1',NS1'是一种保守的预测RNA假结介导的核糖体移码产物。在断奶的ICR小鼠中,SA14-14-2在神经侵袭性和神经毒力方面均高度减毒,肌肉注射和脑内接种时,其半数致死剂量始终比SA14高五个对数以上。有趣的是,SA14-14-2的神经毒力取决于小鼠年龄,1至7日龄小鼠高度易感,14至21日龄小鼠对脑内接种产生抗性。在基因组水平上,SA14-14-2与SA14有57个核苷酸的差异,包括预测的NS1'合成RNA假结内第3599位的一个沉默G到A替换;在这57个差异中,25个导致氨基酸替换。我们的数据为新型基因工程乙脑疫苗的开发铺平了道路。

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