Memory T cells cross-reactive with epitopes encoded by related or even unrelated viruses may alter the immune response and pathogenesis of infection by a process known as heterologous immunity. Because a challenge virus epitope may react with only a subset of the T cell repertoire in a cross-reactive epitope-specific memory pool, the vigorous cross-reactive response may be narrowly focused, or oligoclonal. We show in this article, by examining human T cell cross-reactivity between the HLA-A2-restricted influenza A virus-encoded M1(58-66) epitope (GILGFVFTL) and the dissimilar Epstein-Barr virus-encoded BMLF1(280-288) epitope (GLCTLVAML), that, under some conditions, heterologous immunity can lead to a significant broadening, rather than a narrowing, of the TCR repertoire. We suggest that dissimilar cross-reactive epitopes might generate a broad, rather than a narrow, T cell repertoire if there is a lack of dominant high-affinity clones; this hypothesis is supported by computer simulation.
Broad cross-reactive TCR repertoires recognizing dissimilar Epstein-Barr and influenza A virus epitopes.
具有广泛交叉反应性的 TCR 库,可识别不同的 Epstein-Barr 病毒和甲型流感病毒表位
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作者:Clute Shalyn C, Naumov Yuri N, Watkin Levi B, Aslan Nuray, Sullivan John L, Thorley-Lawson David A, Luzuriaga Katherine, Welsh Raymond M, Puzone Roberto, Celada Franco, Selin Liisa K
| 期刊: | Journal of Immunology | 影响因子: | 3.400 |
| 时间: | 2010 | 起止号: | 2010 Dec 1; 185(11):6753-64 |
| doi: | 10.4049/jimmunol.1000812 | ||
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