具有囊膜蛋白中糖环缺失的寨卡病毒变体的致病性和结构基础。
Pathogenicity and Structural Basis of Zika Variants with Glycan Loop Deletions in the Envelope Protein.
机构信息
Department of Virology, State Key Laboratory of Pathogen and Biosecurity, Beijing Institute of Microbiology and Epidemiology, Academy of Military Medical Sciences, Beijing, China.
School of Basic Medicine, Anhui Medical University, Hefei, China.
出版信息
J Virol. 2022 Dec 14;96(23):e0087922. doi: 10.1128/jvi.00879-22. Epub 2022 Nov 15.
The glycan loop of Zika virus (ZIKV) envelope protein (E) contains the glycosylation site and has been well documented to be important for viral pathogenesis and transmission. In the present study, we report that deletions in the E glycan loop, which were recorded in African ZIKV strains previously, have re-emerged in their contemporary Asian lineages. Here, we generated recombinant ZIKV containing specific deletions in the E glycan loop by reverse genetics. Extensive and characterization of these deletion mutants demonstrated an attenuated phenotype in an adult A129 mouse model and reduced oral infections in mosquitoes. Surprisingly, these glycan loop deletion mutants exhibited an enhanced neurovirulence phenotype, and resulted in a more severe microcephalic brain in neonatal mouse models. Crystal structures of the ZIKV E protein and a deletion mutant at 2.5 and 2.6 Å, respectively, revealed that deletion of the glycan loop induces encephalitic flavivirus-like conformational alterations, including the appearance of perforations on the surface and a clear change in the topology of the loops. Overall, our results demonstrate that the E glycan loop deletions represent neonatal mouse neurovirulence markers of ZIKV. Zika virus (ZIKV) has been identified as a cause of microcephaly and acquired evolutionary mutations since its discovery. Previously deletions in the E glycan loop were recorded in African ZIKV strains, which have re-emerged in the contemporary Asian lineages recently. The glycan loop deletion mutants are not glycosylated, which are attenuated in adult A129 mouse model and reduced oral infections in mosquitoes. More importantly, the glycan loop deletion mutants induce an encephalitic flavivirus-like conformational alteration in the E homodimer, resulting in a significant enhancement of neonatal mouse neurovirulence. This study underscores the critical role of glycan loop deletion mutants in ZIKV pathogenesis, highlighting a need for global virological surveillance for such ZIKV variants.
寨卡病毒(ZIKV)包膜蛋白(E)的聚糖环含有糖基化位点,其对于病毒发病机制和传播至关重要,这已得到充分证实。在本研究中,我们报告称,先前在非洲 ZIKV 株中记录的 E 聚糖环缺失已在其当代亚洲谱系中重新出现。在此,我们通过反向遗传学生成了含有 E 聚糖环特定缺失的重组 ZIKV。对这些缺失突变体的广泛和表征表明,在成年 A129 小鼠模型中表现出减毒表型,并降低了蚊子中的口服感染。令人惊讶的是,这些聚糖环缺失突变体表现出增强的神经毒力表型,并导致新生小鼠模型中更严重的小头畸形脑。ZIKV E 蛋白和缺失突变体的晶体结构分别在 2.5 和 2.6 Å处,揭示了聚糖环缺失诱导脑炎黄病毒样构象改变,包括表面出现穿孔和环拓扑结构的明显变化。总体而言,我们的结果表明,E 聚糖环缺失代表 ZIKV 的新生小鼠神经毒力标志物。寨卡病毒(ZIKV)自发现以来已被确定为小头症的病因,并发生了进化突变。以前在非洲 ZIKV 株中记录的 E 聚糖环缺失最近在当代亚洲谱系中重新出现。聚糖环缺失突变体不发生糖基化,在成年 A129 小鼠模型中减毒,并降低蚊子中的口服感染。更重要的是,聚糖环缺失突变体在 E 同源二聚体中诱导脑炎黄病毒样构象改变,导致新生小鼠神经毒力显著增强。这项研究强调了聚糖环缺失突变体在 ZIKV 发病机制中的关键作用,突显了对这些 ZIKV 变体进行全球病毒学监测的必要性。
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