Examining protective efficacy of influenza virus NA-containing virus-like particles (VLP) in mouse model of post-influenza bacterial pneumonia caused by Staphylococcus aureus
- 作者: Glubokova E.A.1, Leneva I.A.1, Falinskova I.N.1, Poddubikov A.V.1
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隶属关系:
- I. Mechnikov Research Institute for Vaccines and Sera
- 期: 卷 23, 编号 4 (2020)
- 页面: 389-394
- 栏目: SHORT COMMUNICATIONS
- URL: https://journal-vniispk.ru/1028-7221/article/view/120106
- DOI: https://doi.org/10.46235/1028-7221-441-EPF
- ID: 120106
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Currently, pneumonia resulting from post-influenza infection still remains a pressing issue. In particular, virtually no studies regarding a role of immune response against influenza virus neuraminidase in regulating host susceptibility to subsequent bacterial superinfection are now available. Virus-like particles represent one of the new and promising approaches in contemporary virology for developing influenza vaccines and studying influenza virus proteins. Upon that, it is possible to obtain virus-like particles carrying individual influenza virus-derived proteins such as neuraminidase and hemagglutinin. This allows to get closer insight into potential role of individual influenza virus proteins for host immune response as well as assess a risk of developing secondary bacterial pneumonia. In this study we examined an immune response against influenza virus NA protein and its impact in generating resistance to secondary bacterial pneumonia by using neuraminidase-bearing virus-like particles. We used an experimental model of secondary bacterial pneumonia induced by Staphylococcus aureus after influenza infection. Animals were preliminarily vaccinated with virus-like particles carrying neuraminidase, hemagglutinin, or both (a cocktail of virus-like particles). In this model vaccinated animals were infected 21 days later with influenza viruses A/Puerto Rico/8/34 (H1N1) and reassortant strain NIBRG-121xp (A/California/04/2009 (pndm H1N1 2009) X A/Puerto Rico/8/34 ( H1N1) bearing surface proteins hemagglutinin and neuraminidase derived from the A/California/04/2009 virus as well as the internal proteins derived from A/Puerto Rico/8/34. Next, 5 days after influenza infection mice were infected with Staphylococcus aureus. Moreover, animals in one group were simultaneously vaccinated and infected with A/Puerto Rico/8/34 (H1N1) followed by inoculation on day 21 with reassortant virus NIBRG- 121xp. The protective vaccine activity was assessed by measuring survival rate, life expectancy and decreased body weight loss. The data obtained showed that virus-like particles containing neuraminidase revealed no protective activity. However, a cocktail of virus-like particles, containing hemagglutinin and neuraminidase, protected animals from lethal outcome as well as body weight loss. Moreover, the increase virus-like particles containing neuraminidase in the cocktail of virus-like particles (virus-like particles containing neuraminidase + hemagglutinin) led to elevated protective effect after vaccination that was comparable or even superior to that one in mice with post-infectious immunity.
作者简介
E. Glubokova
I. Mechnikov Research Institute for Vaccines and Sera
编辑信件的主要联系方式.
Email: eaglubokova@yandex.ru
Glubokova Ekaterina A. - Junior Research Associate, Laboratory of Experimental Virology, O.G. Anjaparidze Department of Virology
105064, Moscow, Malyi Kazennyi lane, 5a
Phone: 7 (916) 588-55-89
俄罗斯联邦I. Leneva
I. Mechnikov Research Institute for Vaccines and Sera
Email: fake@neicon.ru
I. Falinskova
I. Mechnikov Research Institute for Vaccines and Sera
Email: fake@neicon.ru
Research Associate, Laboratory of Experimental Virology, O.G. Anjaparidze Department of Virology
Moscow
俄罗斯联邦A. Poddubikov
I. Mechnikov Research Institute for Vaccines and Sera
Email: fake@neicon.ru
PhD (Biology), Head, Laboratory of Microbiology of Opportunistic Bacteria, Department of Microbiology
Moscow
俄罗斯联邦参考
- Глубокова Е.А., Вартанова Н.О., Поддубиков А.В., Ленева И.А. Индукция вторичной батериальной пневмонии у мышей, вызываемой различными штаммами Staphylococcus aureus при заражении пандемическим и лабораторным штаммами вируса гриппа H1N1 // Вестник «Биомедицина и социология», 2018. Т. 3, № 3. С. 12-14. [Glubokova E.A., Vartanova N.O., Poddubikov A.V., Leneva I.А. Induction of secondary bacterial pneumonia in mice caused by different strains of S. aureus infected with pandemic and laboratory strains of the H1N1 influenza virus. Vestnik “Biomeditsina i sotsiologiya” = Bulletin “Biomedicine and Sociology”, 2018, Vol. 3, no. 3, pp. 12-14. (In Russ.)]
- Ленева И.А., Егоров А.Ю., Фалынскова И.Н., Махмудова Н.Р., Карташова Н.П., Глубокова Е.А., Вартанова Н.О., Поддубиков А. Индукция вторичной бактериальной пневмонии у мышей при заражении пандемическим и лабораторным штаммами вируса гриппа H1N1 // Журнал микробиологии, эпидемиологии и иммунобиологии, 2019. № 1. С. 68-74. [Leneva I.А., Egorov A.Yu., Falynskova I.N., Makhmudova N.R., Kartashova N., Glubokova E.A., Vartanova N.O., Poddubikov A.V. Induction of secondary bacterial pneumonia in mice upon infection with pandemic and laboratory strains of the H1N1 influenza virus. Zhurnal mikrobiologii, epidemiologii i immunobiologii = Journal of Microbiology, Epidemiology and Immunobiology, 2019, no. 1, pp. 68-74. (In Russ.)]
- Egorov A. The problem of bacterial complications post respiratory viral infections. MIR J., 2018, Vol. 5, no. 1, pp. 12-21.
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