In Vitro Discovery of a Therapeutic Lead for HFMD From a Library Screen of Rocaglates/Aglains

IF 4.6 3区 医学 Q1 VIROLOGY Journal of Medical Virology Pub Date : 2025-02-08 DOI:10.1002/jmv.70228
Adrian Oo, Angel Borge, Regina Ching Hua Lee, Cyrill Kafi Salim, Wenyu Wang, Michael Ricca, Deborah Yuhui Fong, Sylvie Alonso, Lauren E. Brown, John A. Porco Jr., Justin Jang Hann Chu
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Abstract

The lack of effective antiviral treatments for enteroviruses, including human enterovirus A71 (EV-A71), have resulted in an immense global healthcare burden associated with hand-foot-and-mouth disease (HFMD). Rocaglates and aglains belong to a family of compounds produced by Aglaia genus plants. Since the initial discovery of rocaglates in 1982, various rocaglates and aglains have been synthesized and extensively studied mainly as anticancer agents. Here, we report the discovery of a novel aglain derivative as a potential EV-A71 inhibitor. From an immunofluorescence-based phenotypic screen of a library of 296 rocaglate and aglain derivatives, we identified a lead aglain which effectively suppressed EV-A71 replication by 2.3 log fold at a non-cytotoxic concentration, with a host cell CC50 of 21.78 µM, an EV-A71 infection EC50 of 3.57 µM, and a selectivity index of 6.1. Further validation revealed inhibition of EV-A71 across multiple human cell types and a pan-enterovirus inhibitory spectrum against other enteroviruses. Subsequent mechanistic investigation revealed interference with EV-A71 intracellular post-entry events including viral RNA transcription and translation. Findings from this study have established a strong foundation for development of aglain scaffolds as much needed antiviral agents for HFMD, paving the way for future medicinal chemistry optimization and in vivo studies.

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从罗格蛋白库筛选中体外发现治疗手足口病的铅
缺乏有效的肠道病毒抗病毒治疗,包括人类肠道病毒A71 (EV-A71),已导致与手足口病(HFMD)相关的巨大全球卫生保健负担。双头草和双头草是由双头草属植物产生的化合物。自1982年首次发现磁珠酸盐以来,各种磁珠酸盐和磁珠酸盐被合成并广泛研究,主要作为抗癌药物。在这里,我们报告了一种新的aglain衍生物作为潜在的EV-A71抑制剂的发现。通过对296个rocaglate和aglain衍生物库的免疫荧光表型筛选,我们发现一种铅aglain在非细胞毒性浓度下有效抑制EV-A71复制,其宿主细胞CC50为21.78µM, EV-A71感染EC50为3.57µM,选择性指数为6.1。进一步验证显示EV-A71在多种人类细胞类型中具有抑制作用,并且对其他肠道病毒具有泛肠道病毒抑制谱。随后的机制研究发现干扰EV-A71进入细胞后的事件,包括病毒RNA转录和翻译。本研究的发现为开发再蛋白支架作为手足口病急需的抗病毒药物奠定了坚实的基础,为未来的药物化学优化和体内研究铺平了道路。
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来源期刊
Journal of Medical Virology
Journal of Medical Virology 医学-病毒学
CiteScore
23.20
自引率
2.40%
发文量
777
审稿时长
1 months
期刊介绍: The Journal of Medical Virology focuses on publishing original scientific papers on both basic and applied research related to viruses that affect humans. The journal publishes reports covering a wide range of topics, including the characterization, diagnosis, epidemiology, immunology, and pathogenesis of human virus infections. It also includes studies on virus morphology, genetics, replication, and interactions with host cells. The intended readership of the journal includes virologists, microbiologists, immunologists, infectious disease specialists, diagnostic laboratory technologists, epidemiologists, hematologists, and cell biologists. The Journal of Medical Virology is indexed and abstracted in various databases, including Abstracts in Anthropology (Sage), CABI, AgBiotech News & Information, National Agricultural Library, Biological Abstracts, Embase, Global Health, Web of Science, Veterinary Bulletin, and others.
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