I223R Mutation in Influenza A(H1N1)pdm09 Neuraminidase Confers Reduced Susceptibility to Oseltamivir and Zanamivir and Enhanced Resistance with H275Y | Zendy

Jérôme LeGoff | Zendy; Dominique Rousset | Zendy; Georges Abou-Jaoudé | Zendy; Anne Scemla | Zendy; Patricia Ribaud | Zendy; Séverine MercierDelarue | Zendy; Valérie Caro | Zendy; Vincent Enouf | Zendy; François Simon | Zendy; JeanMichel Molina | Zendy; Sylvie van der Werf | Zendy

Open Access

I223R Mutation in Influenza A(H1N1)pdm09 Neuraminidase Confers Reduced Susceptibility to Oseltamivir and Zanamivir and Enhanced Resistance with H275Y

Author(s) -

Jérôme LeGoff,

Dominique Rousset,

Georges Abou-Jaoudé,

Anne Scemla,

Patricia Ribaud,

Séverine MercierDelarue,

Valérie Caro,

Vincent Enouf,

François Simon,

JeanMichel Molina,

Sylvie van der Werf

Publication year - 2012

Publication title -

plos one

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 0.99

H-Index - 332

ISSN - 1932-6203

DOI - 10.1371/journal.pone.0037095

Subject(s) - oseltamivir , zanamivir , neuraminidase , virology , resistance mutation , microbiology and biotechnology , neuraminidase inhibitor , biology , virus , mutation , influenza a virus , medicine , gene , genetics , polymerase chain reaction , reverse transcriptase , covid-19 , disease , pathology , infectious disease (medical specialty)

Background Resistance of pandemic A(H1N1)2009 (H1N1pdm09) virus to neuraminidase inhibitors (NAIs) has remained limited. A new mutation I223R in the neuraminidase (NA) of H1N1pdm09 virus has been reported along with H275Y in immunocompromised patients. The aim of this study was to determine the impact of I223R on oseltamivir and zanamivir susceptibility. Methods The NA enzymatic characteristics and susceptibility to NAIs of viruses harbouring the mutations I223R and H275Y alone or in combination were analyzed on viruses produced by reverse genetics and on clinical isolates collected from an immunocompromised patient with sustained influenza H1N1pdm09 virus shedding and treated by oseltamivir (days 0–15) and zanamivir (days 15–25 and 70–80). Results Compared with the wild type, the NA of recombinant viruses and clinical isolates with H275Y or I223R mutations had about two-fold reduced affinity for the substrate. The H275Y and I223R isolates showed decreased susceptibility to oseltamivir (246-fold) and oseltamivir and zanamivir (8.9- and 4.9-fold), respectively. Reverse genetics assays confirmed these results and further showed that the double mutation H275Y and I223R conferred enhanced levels of resistance to oseltamivir and zanamivir (6195- and 15.2-fold). In the patient, six days after initiation of oseltamivir therapy, the mutation H275Y conferring oseltamivir resistance and the I223R mutation were detected in the NA. Mutations were detected concomitantly from day 6–69 but molecular cloning did not show any variant harbouring both mutations. Despite cessation of NAI treatment, the mutation I223R persisted along with additional mutations in the NA and the hemagglutinin. Conclusions Reduced susceptibility to both oseltamivir and zanamivir was conferred by the I223R mutation which potentiated resistance to both NAIs when associated with the H275Y mutation in the NA. Concomitant emergence of the I223R and H275Y mutations under oseltamivir treatment underlines the importance of close monitoring of treated patients especially those immunocompromised.

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