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利巴韦林和法匹拉韦抗人星状病毒的抗病毒活性。

Antiviral activity of ribavirin and favipiravir against human astroviruses.

机构信息

Department of Pediatrics, Washington University School of Medicine, St Louis, MO, United States.

Department of Pediatrics, Washington University School of Medicine, St Louis, MO, United States.

出版信息

J Clin Virol. 2020 Feb;123:104247. doi: 10.1016/j.jcv.2019.104247. Epub 2019 Dec 17.

Abstract

BACKGROUND

Recent recognition of invasive astrovirus infections, including encephalitis and viremia in humans, have highlighted the need for effective anti-astrovirus therapeutics. However, there is a paucity of data regarding the in vitro activity of broad-spectrum RNA antivirals against astroviruses, including ribavirin and favipiravir.

OBJECTIVES

We quantified the EC50 values for ribavirin and favipiravir against two human astrovirus strains, astrovirus VA1 (VA1) and human astrovirus 4 (HAstV4).

STUDY DESIGN

Caco-2 cells were infected with VA1 or HAstV4 in the presence of ribavirin or favipiravir (dose range 0.1-1000 μM), and the cells were maintained in media containing the drugs for 72 h. Viral RNA was extracted and quantified by qRT-PCR. As a surrogate for cytotoxicity, cellular adenosine triphosphate (ATP) from each drug treatment was also measured.

RESULTS

VA1 replication was inhibited 10-100-fold by both ribavirin (EC50 = 154 μM) and favipiravir (EC50 = 246 μM). In contrast, ribavirin inhibited HAstV4 replication (EC50 = 268 μM) but favipiravir only reduced replication by 44% at the highest dose. Mild reductions in ATP (17-31%) was only observed at the highest concentration of ribavirin (1000 μM) and no significant decrease in ATP was detected for any concentration of favipiravir.

CONCLUSIONS

Ribavirin inhibited both human astrovirus species and favipiravir was only active against VA1. In the future, the in vivo efficacy of these drugs could be tested with development of an animal model of human astrovirus infection.

摘要

背景

最近人们认识到侵袭性星状病毒感染,包括人类的脑炎和病毒血症,突显了开发有效抗星状病毒治疗药物的必要性。然而,关于广谱 RNA 抗病毒药物(包括利巴韦林和法匹拉韦)对星状病毒的体外活性的数据很少。

目的

我们测定了利巴韦林和法匹拉韦对两种人星状病毒株,即星状病毒 VA1(VA1)和人星状病毒 4(HAstV4)的 EC50 值。

研究设计

在利巴韦林或法匹拉韦存在的情况下,用 VA1 或 HAstV4 感染 Caco-2 细胞(剂量范围为 0.1-1000 μM),并在含有药物的培养基中维持细胞 72 小时。用 qRT-PCR 提取和定量病毒 RNA。作为细胞毒性的替代指标,还测量了每种药物处理的细胞三磷酸腺苷(ATP)。

结果

利巴韦林(EC50=154 μM)和法匹拉韦(EC50=246 μM)均能抑制 VA1 复制 10-100 倍。相比之下,利巴韦林抑制了 HAstV4 的复制(EC50=268 μM),但法匹拉韦在最高剂量下仅将复制减少了 44%。仅在利巴韦林的最高浓度(1000 μM)下观察到 ATP 轻度减少(17-31%),而在任何浓度的法匹拉韦下均未检测到 ATP 显著减少。

结论

利巴韦林抑制了两种人类星状病毒,而法匹拉韦仅对 VA1 有效。未来,可以在开发人类星状病毒感染动物模型的基础上,测试这些药物的体内疗效。

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