4.7 Article

Global update on the susceptibilities of human influenza viruses to neuraminidase inhibitors and the cap-dependent endonuclease inhibitor baloxavir, 2017-2018

期刊

ANTIVIRAL RESEARCH
卷 175, 期 -, 页码 -

出版社

ELSEVIER
DOI: 10.1016/j.antiviral.2020.104718

关键词

Influenza; Neuraminidase inhibitor; Baloxavir; Susceptibility; Surveillance; Resistance

资金

  1. Advanced Molecular Detection (AMD) Program, CDC [AMD-77, AMD-102]
  2. National Key Research and Development Program of China [2016YFD0500208]
  3. Francis Crick Institute from Cancer Research UK [FC001030]
  4. Francis Crick Institute from Medical Research Council [FC001030]
  5. Francis Crick Institute from Wellcome Trust [FC001030]
  6. Australian Government, Department of Health
  7. Ministry of Health, Labour and Welfare, Japan [10110400]
  8. JSPS KAKENHI [18K10036]

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The global analysis of neuraminidase inhibitor (NAI) susceptibility of influenza viruses has been conducted since the 2012-13 period. In 2018 a novel cap-dependent endonuclease inhibitor, baloxavir, that targets polymerase acidic subunit (PA) was approved for the treatment of influenza virus infection in Japan and the United States. For this annual report, the susceptibilities of influenza viruses to NAI5 and baloxavir were analyzed. A total of 15409 viruses, collected by World Health Organization (WHO) recognized National Influenza Centers and other laboratories between May 2017 and May 2018, were assessed for phenotypic NAI susceptibility by five WHO Collaborating Centers (CCs). The 50% inhibitory concentration (IC50) was determined for oseltamivir, zanamivir, peramivir and laninamivir. Reduced inhibition (RI) or highly reduced inhibition (HRI) by one or more NAI5 was exhibited by 0.8% of viruses tested (n = 122). The frequency of viruses with RI or HRI has remained low since this global analysis began (2012-13: 0.6%; 2013-14: 1.9%; 2014-15: 0.5%; 2015-16: 0.8%; 2016-17: 0.2%). PA gene sequence data, available from public databases (n = 13523), were screened for amino acid substitutions associated with reduced susceptibility to baloxavir (PA E23G/K/R, PA A36V, PA A37T, PA I38F/M/T/L, PA El 19D, PA E199G): 11 (0.08%) viruses possessed such substitutions. Five of them were included in phenotypic baloxavir susceptibility analysis by two WHO CCs and IC50 values were determined. The PA variant viruses showed 6-17-fold reduced susceptibility to baloxavir. Overall, in the 2017-18 period the frequency of circulating influenza viruses with reduced susceptibility to NAI5 or baloxavir was low, but continued monitoring is important.

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