Genetic tuning of the novel avian influenza A(H7N9) virus during interspecies transmission, China, 2013

Author:

Wang D12,Yang L21,Gao R1,Zhang X3,Tan Y4,Wu A5,Zhu W1,Zhou J1,Zou S1,Li Xiyan1,Sun Y6,Zhang Y7,Liu Y8,Liu T9,Xiong Y10,Xu J11,Chen L12,Weng Y13,Qi X14,Guo J1,Li Xiaodan1,Dong J1,Huang W1,Zhang Y1,Dong L1,Zhao X1,Liu L1,Lu J1,Lan Y1,Wei H1,Xin L1,Chen Y1,Xu C1,Chen T1,Zhu Y1,Jiang T5,Feng Z15,Yang W15,Wang Y15,Zhu H16,Guan Y16,Gao G F15,Li D1,Han J1,Wang S1,Wu G1,Shu Y1

Affiliation:

1. National Institute for Viral Disease Control and Prevention, Chinese Center for Disease Control and Prevention, Key Laboratory for Medical Virology, National Health and Family Planning Commission, Beijing, China

2. These authors contributed equally to this work

3. Shanghai Municipal Disease Control and Prevention, Shanghai, China

4. Guangxi Center for Disease Control and Prevention, Nanning, China

5. Institutes of Biophysics, Chinese Academy of Sciences, Beijing, China

6. Anhui Provincial Disease Control and Prevention, Hefei, China

7. Zhejiang Provincial Disease Control and Prevention, Hangzhou, China

8. Hunan Provincial Disease Control and Prevention, Changsha, China

9. Shandong Provincial Disease Control and Prevention, Jinan, China

10. Jiangxi Provincial Disease Control and Prevention, Nanchang, China

11. Henan Provincial Disease Control and Prevention, Zhengzhou, China

12. Beijing Municipal Disease Control and Prevention, Beijing, China

13. Fujian Provincial Disease Control and Prevention, Fuzhou, China

14. Jiangsu Provincial Disease Control and Prevention, Nanjing, China

15. Chinese Center for Disease Control and Prevention, Beijing, China

16. The University of Hong Kong, Hong Kong SAR, China

Abstract

A novel avian influenza A(H7N9) virus causing human infection emerged in February 2013 in China. To elucidate the mechanism of interspecies transmission, we compared the signature amino acids of avian influenza A(H7N9) viruses from human and non-human hosts and analysed the reassortants of 146 influenza A(H7N9) viruses with full genome sequences. We propose a genetic tuning procedure with continuous amino acid substitutions and reassorting that mediates host adaptation and interspecies transmission. When the early influenza A(H7N9) virus, containing ancestor haemagglutinin (HA) and neuraminidase (NA) genes similar to A/Shanghai/05 virus, circulated in waterfowl and transmitted to terrestrial poultry, it acquired an NA stalk deletion at amino acid positions 69 to 73. Then, receptor binding preference was tuned to increase the affinity to human-like receptors through HA G186V and Q226L mutations in terrestrial poultry. Additional mammalian adaptations such as PB2 E627K were selected in humans. The continual reassortation between H7N9 and H9N2 viruses resulted in multiple genotypes for further host adaptation. When we analysed a potential association of mutations and reassortants with clinical outcome, only the PB2 E627K mutation slightly increased the case fatality rate. Genetic tuning may create opportunities for further adaptation of influenza A(H7N9) and its potential to cause a pandemic.

Publisher

European Centre for Disease Control and Prevention (ECDC)

Subject

Virology,Public Health, Environmental and Occupational Health,Epidemiology

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