Author:
Akauliya Madhav,Gautam Avishekh,Maharjan Sony,Park Byoung Kwon,Kim Jinsoo,Kwon Hyung-Joo
Abstract
Abstract
Background
CD83 is known to regulate lymphocyte maturation, activation, homeostasis, and antibody response to immunization and infection. While CD83 has a major part in B cell function, its role in influenza A virus infection has not yet been investigated.
Methods
We investigated the role of CD83 using C57BL/6J wild type mice and CD83 knockout (KO) mice after intraperitoneal administration of the influenza A/WSN/1933 virus. We analyzed cells of the peritoneal cavity, splenocytes, and cells of the bone marrow with FACS to investigate CD83 expression and cell population change in response to the virus infection. ELISA was performed with sera and peritoneal cavity fluids to detect A/WSN/1933 virus-specific IgG and the subclasses of IgG.
Results
FACS analysis data showed a transient but distinct induction of CD83 expression in the peritoneal B cells of wild type mice. CD83 KO mice exhibited a delayed recovery of B cells in the bone marrow after influenza virus infection and overall, a smaller T cell population compared to wild type mice. The peritoneal cavity and serum of the wild type mice contained a high titer of IgG within 14 days after infection, whereas the CD83 KO mice had a very low titer of IgG.
Conclusions
These results show the importance of CD83 in lymphocytes homeostasis and antibody production during influenza A virus infection.
Funder
National Research Foundation of Korea
Publisher
Springer Science and Business Media LLC
Subject
Infectious Diseases,Virology
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