Prevention of Autoimmunity and Control of Recall Response to Exogenous Antigen by Fas Death Receptor Ligand Expression on T Cells

Imed Mabrouk, Stéphanie Buart, Meriem Hasmim, Christelle Michiels, Elizabeth Connault, Paule Opolon, Gilles Chiocchia, Matthieu Lévi-Strauss, Salem Chouaib, Saoussen Karray

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    Résumé

    Mice with mutations in the gene encoding Fas ligand (FasL) develop lymphoproliferation and systemic autoimmune diseases. However, the cellular subset responsible for the prevention of autoimmunity in FasL-deficient mice remains undetermined. Here, we show that mice with FasL loss on either B or T cells had identical life span as littermates, and both genotypes developed signs of autoimmunity. In addition, we show that T cell-dependent death was vital for the elimination of aberrant T cells and for controlling the numbers of B cells and dendritic cells that dampen autoimmune responses. Furthermore, we show that the loss of FasL on T cells affected the follicular dentritic cell network in the germinal centers, leading to an impaired recall response to exogenous antigen. These results disclose the distinct roles of cellular subsets in FasL-dependent control of autoimmunity and provide further insight into the role of FasL in humoral immunity.

    langue originaleAnglais
    Pages (de - à)922-933
    Nombre de pages12
    journalImmunity
    Volume29
    Numéro de publication6
    Les DOIs
    étatPublié - 19 déc. 2008

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