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日本脑炎病毒的近原子结构揭示了毒力和稳定性的关键决定因素。

Near-atomic structure of Japanese encephalitis virus reveals critical determinants of virulence and stability.

作者信息

Wang Xiangxi, Li Shi-Hua, Zhu Ling, Nian Qing-Gong, Yuan Shuai, Gao Qiang, Hu Zhongyu, Ye Qing, Li Xiao-Feng, Xie Dong-Yang, Shaw Neil, Wang Junzhi, Walter Thomas S, Huiskonen Juha T, Fry Elizabeth E, Qin Cheng-Feng, Stuart David I, Rao Zihe

机构信息

National Laboratory of Macromolecules, Institute of Biophysics, Chinese Academy of Science, Beijing, 100101, China.

Department of Virology, Beijing Institute of Microbiology and Epidemiology, Beijing, 100071, China.

出版信息

Nat Commun. 2017 Apr 26;8(1):14. doi: 10.1038/s41467-017-00024-6.

Abstract

Although several different flaviviruses may cause encephalitis, Japanese encephalitis virus is the most significant, being responsible for thousands of deaths each year in Asia. The structural and molecular basis of this encephalitis is not fully understood. Here, we report the cryo-electron microscopy structure of mature Japanese encephalitis virus at near-atomic resolution, which reveals an unusual "hole" on the surface, surrounded by five encephalitic-specific motifs implicated in receptor binding. Glu138 of E, which is highly conserved in encephalitic flaviviruses, maps onto one of these motifs and is essential for binding to neuroblastoma cells, with the E138K mutation abrogating the neurovirulence and neuroinvasiveness of Japanese encephalitis virus in mice. We also identify structural elements modulating viral stability, notably Gln264 of E, which, when replaced by His264 strengthens a hydrogen-bonding network, leading to a more stable virus. These studies unveil determinants of neurovirulence and stability in Japanese encephalitis virus, opening up new avenues for therapeutic interventions against neurotropic flaviviruses.Japanese encephalitis virus (JEV) is a Flavivirus responsible for thousands of deaths every year for which there are no specific anti-virals. Here, Wang et al. report the cryo-EM structure of mature JEV at near-atomic resolution and identify structural elements that modulate stability and virulence.

摘要

虽然几种不同的黄病毒都可能导致脑炎,但日本脑炎病毒最为严重,每年在亚洲造成数千人死亡。这种脑炎的结构和分子基础尚未完全明确。在此,我们报告了成熟日本脑炎病毒接近原子分辨率的冷冻电子显微镜结构,该结构揭示了病毒表面一个不寻常的“空洞”,其周围环绕着五个与受体结合相关的脑炎特异性基序。E蛋白的Glu138在脑炎黄病毒中高度保守,定位在其中一个基序上,对于与神经母细胞瘤细胞的结合至关重要,E138K突变消除了日本脑炎病毒在小鼠中的神经毒力和神经侵袭性。我们还确定了调节病毒稳定性的结构元件,特别是E蛋白的Gln264,当它被His264取代时会加强氢键网络,从而产生更稳定的病毒。这些研究揭示了日本脑炎病毒神经毒力和稳定性的决定因素,为针对嗜神经性黄病毒的治疗干预开辟了新途径。日本脑炎病毒(JEV)是一种黄病毒,每年导致数千人死亡,目前尚无特效抗病毒药物。在此,王等人报告了成熟JEV接近原子分辨率的冷冻电镜结构,并确定了调节稳定性和毒力的结构元件。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8556/5432033/560c1945b310/41467_2017_24_Fig1_HTML.jpg

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