Drug Susceptibility Profile and Pathogenicity of H7N9 Influenza Virus (Anhui1 Lineage) with R292K Substitution

Overview

Journal Emerg Microbes Infect

Specialty Infectious Diseases

Date 2015 Jun 4

PMID 26038501

Citations 14

Authors

Xiaonan Zhang

Zhigang Song

Jing He

Hui-Ling Yen

Jianhua Li

Zhaoqin Zhu

Di Tian

Wei Wang

Lei Xu

Wencai Guan

Yi Liu

Sen Wang

Bisheng Shi

Wanju Zhang

Boyin Qin

Jialin Cai

Yanmin Wan

Chunhua Xu

Xiaonan Ren

Haili Chen

Lu Liu

Yuqin Yang

Xiaohui Zhou

Wenjiang Zhou

Jianqing Xu

Xiaoyan Zhang

Malik Peiris

Yunwen Hu

Zhenghong Yuan

Affiliations

Soon will be listed here.

Abstract

Neuraminidase inhibitors (NAIs) are the only available licensed therapeutics against human H7N9 influenza virus infections. The emergence of NAI-resistant variants of H7N9viruses with an NA R292K mutation poses a therapeutic challenge. A comprehensive understanding of the susceptibility of these viruses to clinically available NAIs, non-NAIs and their combinations is crucial for effective treatment. In this study, by using limited serial passage and plaque purification, an R292K variant of the Anhui1 lineage was isolated from a patient with clinical evidence of resistance to oseltamivir. In vitro and cell-based assays confirmed a high level of resistance conferred by the R292K mutation to oseltamivir carboxylate and a moderate level of resistance to zanamivir and peramivir. Non-NAI antivirals, such as T-705, ribavirin and NT-300, efficiently inhibited both the variant and the wild-type in cell-based assays. A combination of NAIs and non-NAIs did not exhibit a marked synergistic effect against the R292K variant. However, the combination of two non-NAIs (T-705 and ribavirin) exhibited significant synergism against the mutant virus. In experimentally infected mice, the variant showed delayed onset of symptoms, a reduced viral load and attenuated lethality compared with the wild-type. Our study suggested non-NAIs should be tested clinically for H7N9 patients with a sustained high viral load. Possible drug combination regimens, such as T-705 plus ribavirin, should be further tested in animal models. The pathogenicity and transmissibility of the R292K H7N9 variant should be further assessed with genetically well-characterized pairs of viruses and, most-desirably, with competitive fitness experiments.

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