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多类抗病毒药物在体外对C型人鼻病毒表现出活性。

Multiple classes of antiviral agents exhibit in vitro activity against human rhinovirus type C.

作者信息

Mello Chris, Aguayo Esmeralda, Rodriguez Madeleine, Lee Gary, Jordan Robert, Cihlar Tomas, Birkus Gabriel

机构信息

Gilead Sciences, Foster City, California, USA.

出版信息

Antimicrob Agents Chemother. 2014;58(3):1546-55. doi: 10.1128/AAC.01746-13. Epub 2013 Dec 23.

Abstract

Human rhinovirus type C (HRV-C) is a newly discovered enterovirus species frequently associated with exacerbation of asthma and other acute respiratory conditions. Until recently, HRV-C could not be propagated in vitro, hampering in-depth characterization of the virus replication cycle and preventing efficient testing of antiviral agents. Herein we describe several subgenomic RNA replicon systems and a cell culture infectious model for HRV-C that can be used for antiviral screening. The replicon constructs consist of genome sequences from HRVc15, HRVc11, HRVc24, and HRVc25 strains, with the P1 capsid region replaced by a Renilla luciferase coding sequence. Following transfection of the replicon RNA into HeLa cells, the constructs produced time-dependent increases in luciferase signal that can be inhibited in a dose-dependent manner by known inhibitors of HRV replication, including the 3C protease inhibitor rupintrivir, the nucleoside analog inhibitor MK-0608, and the phosphatidylinositol 4-kinase IIIβ (PI4K-IIIβ) kinase inhibitor PIK93. Furthermore, with the exception of pleconaril and pirodavir, the other tested classes of HRV inhibitors blocked the replication of full-length HRVc15 and HRVc11 in human airway epithelial cells (HAEs) that were differentiated in the air-liquid interface, exhibiting antiviral activities similar to those observed with HRV-16. In summary, this study is the first comprehensive profiling of multiple classes of antivirals against HRV-C, and the set of newly developed quantitative HRV-C antiviral assays represent indispensable tools for the identification and evaluation of novel panserotype HRV inhibitors.

摘要

人鼻病毒C型(HRV-C)是一种新发现的肠道病毒,常与哮喘加重及其他急性呼吸道疾病相关。直到最近,HRV-C仍无法在体外繁殖,这阻碍了对病毒复制周期的深入表征,并妨碍了抗病毒药物的有效测试。在此,我们描述了几种用于HRV-C的亚基因组RNA复制子系统和细胞培养感染模型,可用于抗病毒筛选。复制子构建体由HRVc15、HRVc11、HRVc24和HRVc25毒株的基因组序列组成,P1衣壳区域被海肾荧光素酶编码序列取代。将复制子RNA转染到HeLa细胞后,构建体产生的荧光素酶信号随时间增加,可被HRV复制的已知抑制剂以剂量依赖方式抑制,包括3C蛋白酶抑制剂卢匹那韦、核苷类似物抑制剂MK-0608和磷脂酰肌醇4激酶IIIβ(PI4K-IIIβ)激酶抑制剂PIK93。此外,除了普来可那立和吡罗达韦外,其他测试类别的HRV抑制剂在气液界面分化的人气道上皮细胞(HAEs)中阻断了全长HRVc15和HRVc11的复制,表现出与HRV-16类似的抗病毒活性。总之,本研究是首次对多种类别的抗HRV-C抗病毒药物进行全面分析,新开发的一系列定量HRV-C抗病毒检测方法是鉴定和评估新型泛血清型HRV抑制剂不可或缺的工具。

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