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生成一种稳定的 GFP 报告 Zika 病毒系统,用于高通量筛选 Zika 病毒抑制剂。

Generation of A Stable GFP-reporter Zika Virus System for High-throughput Screening of Zika Virus Inhibitors.

机构信息

State Key Laboratory of Veterinary Biotechnology, Harbin Veterinary Research Institute of Chinese Academy of Agricultural Sciences, Harbin, 150069, China.

Jiangsu Co-Innovation Centre for Prevention and Control of Important Animal Infectious Disease and Zoonoses, Yangzhou University, Yangzhou 225009, China.

出版信息

Virol Sin. 2021 Jun;36(3):476-489. doi: 10.1007/s12250-020-00316-0. Epub 2020 Nov 24.

Abstract

Zika virus (ZIKV) is associated with severe birth defects and Guillain-Barré syndrome and no approved vaccines or specific therapies to combat ZIKV infection are currently available. To accelerate anti-ZIKV therapeutics research, we developed a stable ZIKV GFP-reporter virus system with considerably improved GFP visibility and stability. In this system a BHK-21 cell line expressing DC-SIGNR was established to facilitate the proliferation of GFP-reporter ZIKV. Using this reporter virus system, we established a high-throughput screening assay and screened a selected plant-sourced compounds library for their ability to block ZIKV infection. More than 31 out of 974 tested compounds effectively decreased ZIKV reporter infection. Four selected compounds, homoharringtonine (HHT), bruceine D (BD), dihydroartemisinin (DHA) and digitonin (DGT), were further validated to inhibit wild-type ZIKV infection in cells of BHK-21 and human cell line A549. The FDA-approved chronic myeloid leukemia treatment drug HHT and BD were identified as broad-spectrum flavivirus inhibitors. DHA, another FDA-approved antimalarial drug effectively inhibited ZIKV infection in BHK-21 cells. HHT, BD and DHA inhibited ZIKV infection at a post-entry stage. Digitonin was found to have inhibitory activity in the early stage of viral infection. Our research provides an efficient high-throughput screening assay for ZIKV inhibitors. The active compounds identified in this study represent potential therapies for the treatment of ZIKV infection.

摘要

寨卡病毒(ZIKV)与严重的出生缺陷和格林-巴利综合征有关,目前尚无可用的批准疫苗或针对 ZIKV 感染的特定疗法。为了加速抗 ZIKV 治疗学的研究,我们开发了一种稳定的 ZIKV GFP 报告病毒系统,该系统具有显著提高的 GFP 可见度和稳定性。在该系统中,建立了表达 DC-SIGNR 的 BHK-21 细胞系,以促进 GFP 报告 ZIKV 的增殖。使用该报告病毒系统,我们建立了高通量筛选测定法,并筛选了选定的植物源化合物文库,以评估其阻断 ZIKV 感染的能力。在 974 种测试化合物中,有 31 种以上的化合物能有效降低 ZIKV 报告病毒的感染。四种选定的化合物,即高三尖杉酯碱(HHT)、蝙蝠葛碱 D(BD)、二氢青蒿素(DHA)和瑞香素(DGT),进一步验证了它们在 BHK-21 细胞和人 A549 细胞系中抑制野生型 ZIKV 感染的能力。被 FDA 批准用于治疗慢性髓性白血病的药物 HHT 和 BD 被鉴定为广谱黄病毒抑制剂。另一种被 FDA 批准的抗疟药物 DHA 也能有效抑制 BHK-21 细胞中的 ZIKV 感染。HHT、BD 和 DHA 在进入后阶段抑制 ZIKV 感染。瑞香素被发现对病毒感染的早期阶段具有抑制活性。我们的研究为 ZIKV 抑制剂提供了一种高效的高通量筛选测定法。本研究中鉴定的活性化合物代表了治疗 ZIKV 感染的潜在疗法。

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