Examining immune arms in mice immunized with site-specific influenza virus mutants

S. G. Markushin; N. K. Akhmatova; V. N. Stolpnikova; I. Iv. Akopova; A. A. Rtishchev; E. O. Kalinichenko

doi:10.15789/2220-7619-EIA-1175

Инфекция и иммунитет (May 2020)

Examining immune arms in mice immunized with site-specific influenza virus mutants

S. G. Markushin,
N. K. Akhmatova,
V. N. Stolpnikova,
I. Iv. Akopova,
A. A. Rtishchev,
E. O. Kalinichenko

Affiliations

S. G. Markushin: Mechnikov Research Institute for Vaccines and Sera
N. K. Akhmatova: Mechnikov Research Institute for Vaccines and Sera
V. N. Stolpnikova: Mechnikov Research Institute for Vaccines and Sera
I. Iv. Akopova: Mechnikov Research Institute for Vaccines and Sera
A. A. Rtishchev: Mechnikov Research Institute for Vaccines and Sera
E. O. Kalinichenko: Mechnikov Research Institute for Vaccines and Sera

DOI: https://doi.org/10.15789/2220-7619-EIA-1175
Journal volume & issue: Vol. 10, no. 2
pp. 295 – 304

Abstract

Read online

Site-specific mutants as candidates for live influenza vaccines were resulted from directly introducing into the genome of the pathogenic influenza virus A/WSN/33 (H1N1) strain ts mutations derived from the genes encoding the polymerase complex proteins from some cold-adapted strains serving as attenuation donor. Here we present the data of a comparative study examining immune system arms in mice immunized intranasally with influenza virus mutants and classical cold-adapted reassortant obtained by crossing cold-adapted strain Donor A/Krasnodar/101/35/59 (H2N2) with strain A/WSN/33 (H1N1) bearing surface antigens (hemagglutinin and neuraminidase) similar to mutants. Immunophenotyping mononuclear leukocytes from immunized mice indicated at moderate suppressive effect after using site-specific mutant and the HA reassortant viruses on some immune cell subsets. All viruses in immunized mice resulted in activation of certain lymphocyte subsets including MHC II-positive cells, CD45+/CD19+ B lymphocytes and natural killer cells (CD16/32+/CD3–). Timescale and magnitude of activation markedly differed for each cell subsets. Mice immunized with mutants M26 and U2 peaked with count of CD16/32+/CD3– expressing cells on day 2 after the second immunization compared with control (p < 0.05) that may suggest about an important role for NK cells in activating immune response. In contrast, no significant changes were observed during the study in percentage of CD4+/CD25+/Fox P3 regulatory T cells, CD4+ T helpers and CD8+ cytotoxic cells, except for a sharply decreased count of activated CD4+/CD25+ cells (4-fold) on day 7 after immunization with mutant virus M26. Moreover, mutants U2 and M26 more moderately increased percentage of TLR2- and TLR4-positive cells. The viruses studied ambiguously affected count of TLR9-expressing cells in immunized animals. All viruses increased phagocytic activity in monocytes, but not neutrophils. Despite the moderate activation of innate and adaptive immunity arms, site-specific mutants more profoundly affected humoral reactions inducing increased antibody titers, so that immunogenicity of mutant viruses was higher than that of the cold-adapted reassortant. Thus, the findings hold a promise of using site-specific mutants as live influenza vaccines.

Published in Инфекция и иммунитет

ISSN: 2220-7619 (Print); 2313-7398 (Online)
Publisher: Sankt-Peterburg : NIIÈM imeni Pastera
Country of publisher: Russian Federation
LCC subjects: Medicine: Internal medicine: Infectious and parasitic diseases
Website: https://iimmun.ru/iimm/index

About the journal

Abstract

Keywords