T-cell mimicry of streptococcal M protein and cardiac myosin epitopes by T-cell clones from rheumatic heart disease
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- 作者:Nadia M.J. Ellis ; Ya Li ; William Hildebrand ; Vincent A. Fischetti and Madeleine W. Cunningham
- 关键词:Acute rheumatic fever ; Rheumatic heart disease ; T-cell mimicry ; Pathogenic mechanisms
- 刊名:International Congress Series
- 出版年:2006
- 出版时间:April 2006
- 年:2006
- 卷:1289
- 期:Complete
- 页码:296-299
- 全文大小:70 K
文摘
Mimicry between streptococcal M protein and cardiac myosin is important in the pathogenesis of rheumatic heart disease. M protein specific human T-cell clones derived from rheumatic carditis were crossreactive with human cardiac myosin, and laminin, a valve protein. Among the 11 CD4+ and CD8+ crossreactive T-cell clones, at least six different reactivity patterns were distinguished, suggesting different degrees of crossreactivity and a very diverse T-cell repertoire. The latter was confirmed by a heterogeneous Vβ-gene and CDR3 usage. The HLA-restriction and Th1 cytokine production in response to rM6 protein was preserved when the T-cell clones were stimulated by human cardiac myosin or other α-helical proteins, such as tropomyosin and laminin. The crossreactive human T-cell clones proliferated to B2 and B3A, dominant peptide epitopes in the B-repeat region of streptococcal M protein. In human cardiac myosin, epitopes were demonstrated in the S2 and light meromyosin (LMM) regions. The study of human T-cell clones from rheumatic heart disease revealed potential sites of T-cell mimicry between streptococcal M protein and human cardiac myosin and represents some of the most well-defined T-cell mimicry in human autoimmune disease.