Apoptosis regulators Fas and Bim synergistically control T-lymphocyte homeostatic proliferation
Details
Publication Year 2010-11,Volume 40,Issue #11,Page 3043-3053
Journal Title
EUROPEAN JOURNAL OF IMMUNOLOGY
Publication Type
Journal Article
Abstract
The size of the peripheral T-lymphocyte compartment is governed by complex homeostatic mechanisms that balance T-cell proliferation and death. Proliferation and survival signals are mediated in part by recurrent self-peptide/MHC-TCR interactions and signaling by the common gamma chain-containing cytokine receptors, including those for IL-7 and IL-15. We have previously shown that the death receptor Fas (CD95/APO-1) regulates apoptosis in response to repeated TCR stimulation, whereas the Bcl-2 homology domain 3 -only protein Bim mediates cytokine withdrawal-induced apoptosis. We therefore reasoned that these two molecules might cooperate in the regulation of homeostatic proliferation. In this study, we observe that the combined loss of Fas and Bim synergistically enhances the accumulation of T cells in lymphopenic host mice, and this is particularly pronounced for the unusual CD4 CD8 TCR alpha beta(+) T cells that are characteristic of Fas-deficient (Fas(lpr/lpr)) mice. Our findings demonstrate that these CD4(-)CD8(-)TCR alpha beta(+) T cells arise from homeostatic proliferation of CD8(+) T cells. These studies also underscore the profound rate of baseline T-cell proliferation that likely occurs in wild-type mice even in the absence of foreign antigen, and the consequent need for its coordinated regulation by multiple death-signaling pathways.
Publisher
WILEY-BLACKWELL
Keywords
AUTOIMMUNE LYMPHOPROLIFERATIVE SYNDROME; FAMILY MEMBER BIM; LPR MICE; CELL HOMEOSTASIS; IN-VIVO; RHEUMATOID-ARTHRITIS; BCL-2; NAIVE; SELECTION; DEATH
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Creation Date: 2010-11-01 12:00:00
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