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Статья
Effect of neuraminidase inhibitor-resistant mutationson pathogenicity of clade 2.2 A/Turkey/15/06 (H5N1) influenza virus in Ferrets
2021
The acquisition of neuraminidase (NA) inhibitor resistance by H5N1 influenza viruses has serious clinical implications, as this class of drugs can be an essential component of pandemic control measures. The continuous evolution of the highly pathogenic H5N1 influenza viruses results in the emergence of natural NA gene variations whose impact on viral fitness and NA inhibitor susceptibility are poorly defined. We generated seven genetically stable recombinant clade 2.2 A/Turkey/15/06- like (H5N1) influenza viruses carrying NA mutations located either in the framework residues (E119A, H274Y, N294S) or in close proximity to the NA enzyme active site (V116A, I117V, K150N, Y252H). NA enzyme inhibition assays showed that NA mutations at positions 116, 117, 274, and 294 reduced susceptibility to oseltamivir carboxylate (IC50s increased 5- to 940- fold). Importantly, the E119A NA mutation (previously reported to confer resistance in the N2 NA subtype) was stable in the clade 2.2 H5N1 virus background and induced cross-resistance to oseltamivir carboxylate and zanamivir. We demonstrated that Y252H NA mutation contributed for decreased susceptibility of clade 2.2 H5N1 viruses to oseltamivir carboxylate as compared to clade 1 viruses. The enzyme kinetic parameters (Vmax, Km and Ki) of the avian-like N1 NA glycoproteins were highly consistent with their IC50 values. None of the recombinant H5N1 viruses had attenuated virulence in ferrets inoculated with 106 EID50 dose. Most infected ferrets showed mild clinical disease signs that differed in duration. However, H5N1 viruses carrying the E119A or the N294S NA mutation were lethal to 1 of 3 inoculated animals and were associated with significantly higher virus titers (P<0.01) and inflammation in the lungs compared to the wild-type virus. Our results suggest that highly pathogenic H5N1 variants carrying mutations within the NA active site that decrease susceptibility to NA inhibitors may possess increased virulence in mammalian hosts compared to drug-sensitive viruses. There is a need for novel anti-influenza drugs that target different virus/host factors and can limit the emergence of resistance. © 2010 Ilyushina et al.
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Версии
- 1. Version of Record от 2021-04-27
Метаданные
Название журнала
- PLoS Pathogens
Том
- 6
Выпуск
- 5
Страницы
- 1-11
Ключевые слова
- 4 acetamido 5 amino 3 (1 ethylpropoxy) 1 cyclohexene 1 carboxylic acid; sialidase; sialidase inhibitor; virus glycoprotein; virus RNA; zanamivir; antivirus agent; drug derivative; enzyme inhibitor; oseltamivir; recombinant protein; sialidase; zanamivir; animal cell; animal experiment; animal model; animal tissue; antiviral resistance; antiviral susceptibility; article; cell strain HEK293; cladistics; controlled study; cross resistance; disease duration; disease severity; drug targeting; enzyme active site; enzyme inhibition; enzyme kinetics; ferret; genetic stability; genetic variability; histopathology; human; human cell; IC 50; influenza A (H5N1); Influenza virus A H5N1; kidney cell; male; molecular evolution; nonhuman; pneumonia; virus load; virus mutation; virus recombinant; virus virulence; wild type; animal; cell line; chemistry; crystallography; cytology; disease model; dog; drug antagonism; genetics; immunology; Influenza virus A H5N1; kidney; orthomyxovirus infection; pathogenicity; protein tertiary structure; virology; Animalia; Aves; Mammalia; Mustela; Orthomyxoviridae; Animals; Antiviral Agents; Cell Line; Crystallography; Disease Models, Animal; Dogs; Drug Resistance, Viral; Enzyme Inhibitors; Ferrets; Humans; Influenza A Virus, H5N1 Subtype; Kidney; Male; Neuraminidase; Orthomyxoviridae Infections; Oseltamivir; Protein Structure, Tertiary; Recombinant Proteins; Zanamivir
Издатель
- Public Library of Science
Тип документа
- journal article
Тип лицензии Creative Commons
- CC
Правовой статус документа
- Свободная лицензия
Источник
- scopus
