Exosomes Released by Influenza-Virus-Infected Cells Carry Factors Capable of Suppressing Immune Defense Genes in Naïve Cells

Yana Zabrodskaya; Marina Plotnikova; Nina Gavrilova; Alexey Lozhkov; Sergey Klotchenko; Artem Kiselev; Vladimir Burdakov; Edward Ramsay; Lada Purvinsh; Marja Egorova; Vera Vysochinskaya; Irina Baranovskaya; Alexandra Brodskaya; Roman Povalikhin; Andrey Vasin

doi:10.3390/v14122690

Exosomes Released by Influenza-Virus-Infected Cells Carry Factors Capable of Suppressing Immune Defense Genes in Naïve Cells

Viruses. 2022 Nov 30;14(12):2690. doi: 10.3390/v14122690.

Authors

Yana Zabrodskaya^{1

2}, Marina Plotnikova², Nina Gavrilova^{1

2}, Alexey Lozhkov^{1

2}, Sergey Klotchenko^{1

2}, Artem Kiselev³, Vladimir Burdakov⁴, Edward Ramsay⁵, Lada Purvinsh⁶, Marja Egorova², Vera Vysochinskaya^{1

2}, Irina Baranovskaya^{2

7}, Alexandra Brodskaya^{1

2}, Roman Povalikhin¹, Andrey Vasin^{1

2}

Affiliations

¹ Institute of Biomedical Systems and Biotechnology, Peter the Great Saint Petersburg Polytechnic University, 29 Ulitsa Polytechnicheskaya, 194064 St. Petersburg, Russia.
² Smorodintsev Research Institute of Influenza, 15/17 Ulitsa Professora Popova, 197376 St. Petersburg, Russia.
³ Institute for Quantitative Health Science and Engineering (IQ), Michigan State University, 775 Woodlot Dr, East Lansing, MI 48824, USA.
⁴ Petersburg Nuclear Physics Institute Named by B. P. Konstantinov of National Research Center, Kurchatov Institute, 1 mkr. Orlova roshcha, 188300 Gatchina, Russia.
⁵ Saint Petersburg Pasteur Institute, 14 Ulitsa Mira, 197101 St. Petersburg, Russia.
⁶ Biology Science Department, The University of Chicago, 947 E. 58th St., Chicago, IL 60637, USA.
⁷ Department of Physiology, Augusta University, 1462 Laney Walker Blvd, CA-3149, Augusta, GA 30912, USA.

Abstract

Background: Exosomes are involved in intercellular communication and can transfer regulatory molecules between cells. Consequently, they can participate in host immune response regulation. For the influenza A virus (IAV), there is very limited information on changes in exosome composition during cell infection shedding light on the potential role of these extracellular membrane vesicles. Thus, the aim of our work was to study changes in exosomal composition following IAV infection of cells, as well as to evaluate their effect on uninfected cells. Methods: To characterize changes in the composition of cellular miRNAs and mRNAs of exosomes during IAV infection of A549 cells, NGS was used, as well as PCR to identify viral genes. Naïve A549 cells were stimulated with infected-cell-secreted exosomes for studying their activity. Changes in the expression of genes associated with the cell's immune response were shown using PCR. The effect of exosomes on IAV replication was shown in MDCK cells using In-Cell ELISA and PCR of the supernatants. Results: A change in the miRNA composition (miR-21-3p, miR-26a-5p, miR-23a-5p, miR-548c-5p) and mRNA composition (RPL13A, MKNK2, TRIB3) of exosomes under the influence of the IAV was shown. Many RNAs were involved in the regulation of the immune response of the cell, mainly by suppressing it. After exosome stimulation of naïve cells, a significant decrease in the expression of genes involved in the immune response was shown (RIG1, IFIT1, MDA5, COX2, NFκB, AnxA1, PKR, IL6, IL18). When infecting MDCK cells, a significant decrease in nucleoprotein levels was observed in the presence of exosomes secreted by mock-infected cells. Viral levels in supernatants also decreased. Conclusions: Exosomes secreted by IAV-infected cells could reduce the immune response of neighboring intact cells, leading to more effective IAV replication. This may be associated both with regulatory functions of cellular miRNAs and mRNAs carried by exosomes, or with the presence of viral mRNAs encoding proteins with an immunosuppressive function.

Keywords: A549 cells; exosome isolation; exosomes; immunosuppression; influenza virus.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

A549 Cells
Exosomes* / metabolism
Humans
Influenza A virus* / genetics
Influenza, Human* / metabolism
MicroRNAs* / genetics
MicroRNAs* / metabolism

Substances

MicroRNAs

Grants and funding

This work was supported by the Russian Science Foundation grant No. 20-15-00228.