Induction of Autoimmune Valvular Heart Disease by Recombinant Streptococcal M Protein

Author:

Quinn Anthony1,Kosanke Stanley2,Fischetti Vincent A.3,Factor Stephen M.4,Cunningham Madeleine W.1

Affiliation:

1. Departments of Microbiology and Immunology1 and

2. Department of Pathology,2 University of Oklahoma Health Sciences Center, Oklahoma City, Oklahoma, and

3. Laboratory of Bacterial Pathogenesis, Rockefeller University, New York,3 and

4. Department of Pathology, Albert Einstein College of Medicine and Jacobi Medical Center, Bronx,4 New York

Abstract

ABSTRACT Rheumatic heart disease is an autoimmune sequela of group A streptococcal infection. Previous studies have established that streptococcal M protein is structurally and immunologically similar to cardiac myosin, a well-known mediator of inflammatory heart disease. In this study, we investigated the hypothesis that streptococcal M protein could produce inflammatory valvular heart lesions similar to those seen in rheumatic fever (RF). Fifty percent (3 of 6) of Lewis rats immunized with recombinant type 6 streptococcal M protein (rM6) developed valvulitis as well as focal lesions of myocarditis. Valvular lesions initiated at the valve surface endothelium spread into the valve. Anitschkow cells and verruca-like lesions were present. T cells from rM6-immunized rats proliferated in the presence of purified cardiac myosin, but not skeletal myosin. A T-cell line produced from rM6-treated rats proliferated in the presence of cardiac myosin and rM6 protein. The study demonstrates that the Lewis rat is a model of valvular heart disease and that streptococcal M protein can induce an autoimmune cell-mediated immune attack on the heart valve in an animal model. The data support the hypothesis that a bacterial antigen can break immune tolerance in vivo, an important concept in autoimmunity.

Publisher

American Society for Microbiology

Subject

Infectious Diseases,Immunology,Microbiology,Parasitology

Reference29 articles.

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3. Resurgence of rheumatic fever in the United States;Ayoub E. M.;Postgrad. Med.,1992

4. Coligan J. E. Kruisbeck A. D. Margulies D. H. Shevach E. M. Strober W. Current protocols in immunology 1 section 3.12 1994 Greene Publishing and Wiley-Interscience New York N.Y

5. Pathogenesis of Group A Streptococcal Infections

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