Etoposide targets 2A protease to inhibit enterovirus 71 replication.

IF 3.7 2区 生物学 Q2 MICROBIOLOGY Microbiology spectrum Pub Date : 2024-11-18 DOI:10.1128/spectrum.02200-24
Qinqin Liang, Sai Shi, Qingjie Zhang, Yaxin Wang, Sheng Ye, Binghong Xu
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Abstract

Enterovirus 71 (EV71) is a major pathogen that causes hand, foot, and mouth disease (HFMD) in infants and children. Notably, no clinically approved drugs specifically target EV71. The EV71 2A protease (2Apro), a cysteine protease produced by the virus, is essential for the virus' replication and has a significant impact on the functioning of host cells. Thus, it presents a valuable target for the discovery of antiviral medications. In this study, based on the monomers and their derivatives in the Library of Traditional Chinese Medicine (TCM), we performed virtual screening and biological experiments. We identified a derivative of a traditional herbal monomer, Etoposide, commonly isolated from the roots and rhizomes of Podophyllum spp. Etoposide inhibited replication of EV71 A, B, C, and CVA16 viruses in a concentration-dependent manner in a variety of cell lines with minimal cytotoxicity. Furthermore, both molecular dynamics simulations and site-directed mutagenesis assays revealed that Etoposide inhibited the activity of the EV71 2A protease by mainly binding to two residues, Y89 and P107. The findings indicate that Etoposide serves as a promising inhibitor of the EV71 2Apro, demonstrating strong antiviral properties and positioning itself as a formidable candidate for clinical trials against EV71.IMPORTANCEWe first used a drug screening approach focused on monomeric compounds and their derivatives from traditional Chinese medicine to identify an EV71 2Apro inhibitor-Etoposide. We then performed biological experiments to validate that Etoposide suppresses the replication of the EV71 virus in a concentration-dependent manner with minimal cytotoxicity to various cell lines. Remarkably, it shows inhibitory activity against EV71 A, B, C, and CVA16, suggesting that Etoposide may be a potential broad-spectrum inhibitor. We revealed a novel mechanism that Etoposide inhibits EV71 proliferation by targeting 2Apro, and the interactions with Y89 and P107 are of great importance. The findings suggest that Etoposide serves as a promising inhibitor of EV71 2Apro, demonstrating significant antiviral properties. It stands out as a strong candidate for broad-spectrum applications in clinical research.

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依托泊苷针对 2A 蛋白酶抑制肠病毒 71 的复制。
肠道病毒 71(EV71)是导致婴幼儿手足口病(HFMD)的主要病原体。值得注意的是,目前还没有临床批准的药物专门针对 EV71。EV71 2A 蛋白酶(2Apro)是病毒产生的一种半胱氨酸蛋白酶,是病毒复制所必需的,并对宿主细胞的功能产生重大影响。因此,它是发现抗病毒药物的一个重要靶点。在本研究中,我们以中药库中的单体及其衍生物为基础,进行了虚拟筛选和生物学实验。我们发现了一种传统中药单体的衍生物--依托泊苷,它通常从鬼臼属植物的根和根茎中分离出来。依托泊苷能以浓度依赖的方式抑制 EV71 A、B、C 和 CVA16 病毒在多种细胞系中的复制,且细胞毒性极低。此外,分子动力学模拟和定点突变试验显示,依托泊苷主要通过与两个残基(Y89 和 P107)结合来抑制 EV71 2A 蛋白酶的活性。研究结果表明,依托泊苷是一种很有前景的EV71 2A蛋白酶抑制剂,具有很强的抗病毒特性,是针对EV71病毒进行临床试验的有力候选药物。我们首先利用药物筛选方法,重点从传统中药中的单体化合物及其衍生物中找出了一种EV71 2A蛋白酶抑制剂--依托泊苷。然后,我们进行了生物学实验,验证了依托泊苷能以浓度依赖性方式抑制 EV71 病毒的复制,且对各种细胞株的细胞毒性极小。值得注意的是,它对 EV71 A、B、C 和 CVA16 均有抑制活性,这表明依托泊苷可能是一种潜在的广谱抑制剂。我们揭示了依托泊苷通过靶向2Apro抑制EV71增殖的新机制,其中与Y89和P107的相互作用非常重要。研究结果表明,依托泊苷是一种很有前途的 EV71 2Apro 抑制剂,具有显著的抗病毒特性。它是临床研究中广谱应用的有力候选药物。
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来源期刊
Microbiology spectrum
Microbiology spectrum Biochemistry, Genetics and Molecular Biology-Genetics
CiteScore
3.20
自引率
5.40%
发文量
1800
期刊介绍: Microbiology Spectrum publishes commissioned review articles on topics in microbiology representing ten content areas: Archaea; Food Microbiology; Bacterial Genetics, Cell Biology, and Physiology; Clinical Microbiology; Environmental Microbiology and Ecology; Eukaryotic Microbes; Genomics, Computational, and Synthetic Microbiology; Immunology; Pathogenesis; and Virology. Reviews are interrelated, with each review linking to other related content. A large board of Microbiology Spectrum editors aids in the development of topics for potential reviews and in the identification of an editor, or editors, who shepherd each collection.
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