IMMUNOPATHOGENESIS OF EXPERIMENTAL COXSACKIE-VIRUS INDUCED MYOCARDITIS - ROLE OF AUTOIMMUNITY
- 1 January 1985
- journal article
- research article
- Vol. 10 (1) , 1-7
Abstract
The pathogenesis of cardiac injury in clinical myocarditis is unknown. Despite the association of the disease with recent viral infections, it is now assumed that immune rather than viral mechanisms are primarily responsible for myocyte destruction. Nonetheless, immunosuppressive therapy has not been universally effective in limiting myocardial damage. To better understand the mechanisms by which viral infections of the heart induce myocarditis, it has been necessary to resort to a murine model of the disease. When inbred Balb/c mice are infected with a cardiotropic variant of Coxsackievirus, group B, type 3 (CVB3), the animals develop extensive interstitial and focal inflammatory cell infiltration of the heart similar to the lesions in humans. As in humans, a number of factors influence the severity of the disease. Males develop severe myocarditis while virgin females are generally protected. Female resistance does not persist during pregnancy, however, when resultant myocarditis is frequently worse than that observed in males. The susceptibility of males and pregnant females results from the influence of testosterone and progesterone on the immune response. Susceptible animals generate autoimmune cytolytic T lymphocytes which recognize normal myocyte cell surface antigens and are responsible for most of the cardiac damage in experimental myocarditis. Virgin females do not develop significant myocarditis apparently because the estrogens enhance suppressor cells which prevent the autoimmune T cell generation. Humoral (antibody-mediated) immunity to the heart antigens is also present, but apparently has no role in the pathogenesis of the disease. Thus, the animal model has been successful in identifying probable mechanisms of cardiac injury in myocarditis and explaining certain epidemiological observations. If the murine model validly reflects the human disease, it might be possible to develop more effective diagnostic and therapeutic procedures.This publication has 18 references indexed in Scilit:
- A rapid solid-phase enzyme-linked binding assay for screening monoclonal antibodies to cell surface antigensJournal of Immunological Methods, 1981
- Interleukin-2 induction of hapten-specific cytolytic T cells in nude mice.The Journal of Immunology, 1981
- Coxsackie B3 Myocarditis in Athymic MiceExperimental Biology and Medicine, 1981
- Defective in vitro suppressor cell function in idiopathic congestive cardiomyopathy.Circulation, 1979
- IDIOPATHIC CARDIOMYOPATHY, AGE, AND SUPPRESSOR-CELL DYSFUNCTION AS RISK DETERMINANTS OF LYMPHOMA AFTER CARDIAC TRANSPLANTATIONThe Lancet, 1978
- MYOCARDIAL CHANGES AFTER INFECTION WITH COXSACKIE VIRUS-B3 IN NUDE-MICE1978
- GENERATION OF CYTOTOXIC T LYMPHOCYTES DURING COXSACKIE-VIRUS B-3 INFECTION .1. MODEL AND VIRAL SPECIFICITY1977
- Separation of helper T cells from suppressor T cells expressing different Ly components. II. Activation by antigen: after immunization, antigen-specific suppressor and helper activities are mediated by distinct T-cell subclasses.The Journal of Experimental Medicine, 1976
- Chronic pernicious myocarditisAmerican Heart Journal, 1960
- ENDOCRINES AND THEIR RELATION TO INFLUENZA VIRUS INFECTIONThe Journal of Experimental Medicine, 1951