Publikation: Antagonistic and synergistic effects of glucocorticoids and IL-7 on CD4+ T cell activation
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Glucocorticoids (GCs) are steroidal compounds widely used to treat chronic and acute inflammatory diseases. In particular, GCs at pharmacological doses induce apoptosis of activated and naïve T cells, inhibit their proliferation and block pro-inflammatory cytokine secretion. At physiological concentrations, the effect of these steroids on T cell immunity are not yet fully understood, and various studies reported paradoxical roles exerted by GCs on T cell immunity. Here, we show that GCs surprisingly induce proliferation of activated CD4+ T cells in the presence of IL-7, a cytokine secreted in the thymus and at mucosal sites. Increased proliferation is dependent on a GC-mediated survival of mitotic cells. Moreover, we observe a downmodulation of Th1 cytokine secretion in cells treated with GCs, an outcome which is not affected by the presence of IL-7. GCs exert thus a positive role in the presence of IL-7 by enhancing proliferation of CD4+ T cells and simultaneously a negative role by suppressing pro-inflammatory cytokine production.
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CIMA, Igor, Andrea FUHRER, Thomas BRUNNER, 2006. Antagonistic and synergistic effects of glucocorticoids and IL-7 on CD4+ T cell activation. In: Immunology Letters. 2006, 106(1), pp. 99-102. ISSN 0165-2478. Available under: doi: 10.1016/j.imlet.2006.04.005BibTex
@article{Cima2006-07-15Antag-14276,
year={2006},
doi={10.1016/j.imlet.2006.04.005},
title={Antagonistic and synergistic effects of glucocorticoids and IL-7 on CD4+ T cell activation},
number={1},
volume={106},
issn={0165-2478},
journal={Immunology Letters},
pages={99--102},
author={Cima, Igor and Fuhrer, Andrea and Brunner, Thomas}
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<dcterms:abstract xml:lang="eng">Glucocorticoids (GCs) are steroidal compounds widely used to treat chronic and acute inflammatory diseases. In particular, GCs at pharmacological doses induce apoptosis of activated and naïve T cells, inhibit their proliferation and block pro-inflammatory cytokine secretion. At physiological concentrations, the effect of these steroids on T cell immunity are not yet fully understood, and various studies reported paradoxical roles exerted by GCs on T cell immunity. Here, we show that GCs surprisingly induce proliferation of activated CD4+ T cells in the presence of IL-7, a cytokine secreted in the thymus and at mucosal sites. Increased proliferation is dependent on a GC-mediated survival of mitotic cells. Moreover, we observe a downmodulation of Th1 cytokine secretion in cells treated with GCs, an outcome which is not affected by the presence of IL-7. GCs exert thus a positive role in the presence of IL-7 by enhancing proliferation of CD4+ T cells and simultaneously a negative role by suppressing pro-inflammatory cytokine production.</dcterms:abstract>
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