Yun Sang-Im, Song Byung-Hak, Kim Jin-Kyoung, Yun Gil-Nam, Lee Eun-Young, Li Long, Kuhn Richard J, Rossmann Michael G, Morrey John D, Lee Young-Min
Department of Animal, Dairy, and Veterinary Sciences; Utah Science Technology and Research, College of Agriculture and Applied Sciences, Utah State University, Logan, Utah, United States of America.
Department of Microbiology, College of Medicine, Chungbuk National University, Cheongju, Republic of Korea.
PLoS Pathog. 2014 Jul 31;10(7):e1004290. doi: 10.1371/journal.ppat.1004290. eCollection 2014 Jul.
Japanese encephalitis virus (JEV), a mosquito-borne flavivirus that causes fatal neurological disease in humans, is one of the most important emerging pathogens of public health significance. JEV represents the JE serogroup, which also includes West Nile, Murray Valley encephalitis, and St. Louis encephalitis viruses. Within this serogroup, JEV is a vaccine-preventable pathogen, but the molecular basis of its neurovirulence remains unknown. Here, we constructed an infectious cDNA of the most widely used live-attenuated JE vaccine, SA14-14-2, and rescued from the cDNA a molecularly cloned virus, SA14-14-2MCV, which displayed in vitro growth properties and in vivo attenuation phenotypes identical to those of its parent, SA14-14-2. To elucidate the molecular mechanism of neurovirulence, we selected three independent, highly neurovirulent variants (LD50, <1.5 PFU) from SA14-14-2MCV (LD50, >1.5×105 PFU) by serial intracerebral passage in mice. Complete genome sequence comparison revealed a total of eight point mutations, with a common single G1708→A substitution replacing a Gly with Glu at position 244 of the viral E glycoprotein. Using our infectious SA14-14-2 cDNA technology, we showed that this single Gly-to-Glu change at E-244 is sufficient to confer lethal neurovirulence in mice, including rapid development of viral spread and tissue inflammation in the central nervous system. Comprehensive site-directed mutagenesis of E-244, coupled with homology-based structure modeling, demonstrated a novel essential regulatory role in JEV neurovirulence for E-244, within the ij hairpin of the E dimerization domain. In both mouse and human neuronal cells, we further showed that the E-244 mutation altered JEV infectivity in vitro, in direct correlation with the level of neurovirulence in vivo, but had no significant impact on viral RNA replication. Our results provide a crucial step toward developing novel therapeutic and preventive strategies against JEV and possibly other encephalitic flaviviruses.
日本脑炎病毒(JEV)是一种由蚊子传播的黄病毒,可导致人类致命的神经系统疾病,是具有公共卫生意义的最重要的新兴病原体之一。JEV属于乙脑血清群,该血清群还包括西尼罗河病毒、墨累谷脑炎病毒和圣路易斯脑炎病毒。在这个血清群中,JEV是一种可通过疫苗预防的病原体,但其神经毒力的分子基础仍然未知。在此,我们构建了最广泛使用的减毒活乙脑疫苗SA14-14-2的感染性cDNA,并从该cDNA中拯救出一种分子克隆病毒SA14-14-2MCV,其在体外的生长特性和在体内的减毒表型与其亲本SA14-14-2相同。为了阐明神经毒力的分子机制,我们通过在小鼠中连续脑内传代,从SA14-14-2MCV(半数致死剂量,>1.5×105 PFU)中筛选出三个独立的、高神经毒力的变体(半数致死剂量,<1.5 PFU)。完整基因组序列比较显示共有8个点突变,其中一个共同的单碱基G1708→A替换导致病毒E糖蛋白第244位的甘氨酸被谷氨酸取代。利用我们的感染性SA14-14-2 cDNA技术,我们表明E-244位点的这一单甘氨酸到谷氨酸的变化足以在小鼠中赋予致命的神经毒力,包括病毒在中枢神经系统中快速传播和组织炎症的发展。对E-244进行全面的定点诱变,并结合基于同源性的结构建模,证明了E-244在JEV神经毒力中在E二聚化结构域的ij发夹内具有新的重要调节作用。在小鼠和人类神经元细胞中,我们进一步表明E-244突变改变了JEV在体外的感染性,这与体内神经毒力水平直接相关,但对病毒RNA复制没有显著影响。我们的结果为开发针对JEV以及可能针对其他脑炎黄病毒的新型治疗和预防策略迈出了关键一步。
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