Asynchronous differentiation of CD8 T cells that recognize dominant and cryptic antigens

Chantal Baron, Marie Christine Meunier, Étienne Caron, Caroline Côté, Mark J. Cameron, David J. Kelvin, Richard LeBlanc, Vincent Rineau, Claude Perreault

Résultat de recherche: Articleexamen par les pairs

9 Citations (Scopus)

Résumé

Restriction of T cell responses to a few epitopes (immunodominance) is a central feature of immune responses. We analyzed the entire transcriptome of effector CD8 T cells specific for a dominant (H7a) and a cryptic (HY) mouse Ag and performed a longitudinal analysis of selected T cell differentiation markers. We found that Ag specificity had a relatively modest influence on the repertoire of genes that are transcriptionally modulated by the CD8 T cell differentiation program. Although the differentiation programs of anti-H7a and anti-HY T cells were similar, they did not progress simultaneously. The expansion peak of anti-H7a T cells was reached on day 10 while that of anti-HY T cells was attained on days 15-20. Between days 10 and 20, anti-H7a T cells were in the contraction phase and anti-HY T cells in the expansion phase. Furthermore, expansion and development of effector function were well-synchronized in anti-H7a T cells but were disconnected in anti-HY T cells. We propose that, by leading to selective expansion of the fittest CD8 T cells, immnnodominance may be beneficial to the host. Inhibition of the T cell response to cryptic Ag would ensure that host resources (APC, cytokines) for which T cells compete are devoted to T cells with the best effector potential. One implication is that favoring expansion of the fittest effector T cells in general may be more important than increasing the diversity of the T cell repertoire.

Langue d'origineEnglish
Pages (de-à)8466-8475
Nombre de pages10
JournalJournal of Immunology
Volume177
Numéro de publication12
DOI
Statut de publicationPublished - déc. 15 2006
Publié à l'externeOui

ASJC Scopus Subject Areas

  • Immunology and Allergy
  • Immunology

PubMed: MeSH publication types

  • Journal Article
  • Research Support, Non-U.S. Gov't

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