Neonatal Infection of Mice With Lactate Dehydrogenase-elevating Virus Results in Suppression of Humoral Antiviral Immune Response but does not Alter the Course of Viraemia or the Polyclonal Activation of B Cells and Immune Complex Formation

Department of Microbiology, Medical School, University of Minnesota, Minneapolis, Minnesota 55455, U.S.A. Neonatal infection of FVB mice with lactate dehydrogenase-elevating virus (LDV) prevented the normal formation of anti-LDV antibodies observed in mice infected at 5 days of age or older. Even 22...

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Bibliographic Details
Published in:Journal of general virology 1994-05, Vol.75 (5), p.1071-1081
Main Authors: Rowland, Raymond R. R, Even, Chen, Anderson, Grant W, Chen, Zongyu, Hu, Bugen, Plagemann, Peter G. W
Format: Article
Language:English
Subjects:
Animals
Animals, Newborn
Antibodies, Viral - blood
Antibody Formation
Antigen-Antibody Complex - blood
Arterivirus Infections - immunology
B-Lymphocytes - immunology
Biological and medical sciences
Cyclophosphamide - pharmacology
Dexamethasone - pharmacology
Experimental viral diseases and models
Fundamental and applied biological sciences. Psychology
Immune Tolerance
Immunity, Cellular
Immunoglobulin G - biosynthesis
Immunoglobulin G - immunology
Infectious diseases
lactate dehydrogenase-elevating virus
Lactate dehydrogenase-elevating virus - growth & development
Lactate dehydrogenase-elevating virus - immunology
Lymphocyte Activation
Macrophages, Peritoneal - drug effects
Macrophages, Peritoneal - immunology
Medical sciences
Mice
Microbiology
Replicative cycle, interference, host-virus relations, pathogenicity, miscellaneous strains
Thymus Gland - microbiology
Viral diseases
Viremia - immunology
Virology
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Summary:Department of Microbiology, Medical School, University of Minnesota, Minneapolis, Minnesota 55455, U.S.A. Neonatal infection of FVB mice with lactate dehydrogenase-elevating virus (LDV) prevented the normal formation of anti-LDV antibodies observed in mice infected at 5 days of age or older. Even 22 weeks post-infection, the concentration of circulating anti-LDV antibodies in neonatally infected mice was insignificant. However, the time course and level of persistent viraemia were the same in neonatally infected mice lacking anti-LDV antibodies as in mice infected at 5 or 15 days of age which developed normal antiviral immune responses. The results support the view that LDV replication in mice is unaffected by antiviral immune responses and instead is primarily dependent on the rate of regeneration of LDV-permissive macrophages. This view is further supported by the following findings. Treatment of mice with cyclophosphamide or dexamethasone, which are known to increase plasma LDV levels, increased the proportion of LDV-permissive macrophages in the peritoneum. Injection of mice with interleukin-3, which is known to stimulate macrophage development, increased plasma LDV levels in persistently infected mice 10- to 100-fold. During the first month of age when mice possess a higher proportion of LDV-permissive macrophages than older mice and peritoneal macrophages exhibit self-sustained growth, the persistent plasma LDV titres were also 10- to 100-fold higher than in older mice. The polyclonal activation of B cells induced by LDV that results in a permanent elevation of IgG2a or IgG2b in the circulation, and the formation of 180K to 300K immune complexes containing IgG2a or IgG2b were also the same in neonatally infected mice and mice infected 5 or 15 days after birth. Thus, the polyclonal activation of B cells occurs in the absence of an antiviral humoral immune response and the immune complexes do not contain anti-LDV antibodies. The immune complexes probably consist of autoantibodies formed in the course of the polyclonal activation of B cells and their cellular antigens. Received 13 September 1993; accepted 26 November 1993.
ISSN:0022-1317
1465-2099
DOI:10.1099/0022-1317-75-5-1071