Newly discovered role for Fas ligand in the cell-cycle arrest of CD4+ T cells

被引:0
|
作者
Julie Desbarats
Richard C. Duke
M. Karen Newell
机构
[1] Division of Immunobiology,Departments of Medicine and Immunology
[2] Department of Medicine University of Vermont College of Medicine,undefined
[3] Shreve Laboratory for Tumor Immunology,undefined
[4] University of Colorado Cancer Center,undefined
来源
Nature Medicine | 1998年 / 4卷
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摘要
Fas Ligand (FasL) can induce apoptosis of Fas-bearing cells. It is expressed on the cell surface of many tumor cells, immune-privileged tissues and activated lymphocytes. We report here that FasL can itself transduce signals, leading to cell-cycle arrest and cell death in CD4+ T cells. In vitro, FasL engagement inhibited CD4+ T-cell proliferation, cell-cycle progression, and IL-2 secretion. In vivo, FasL engagement prevented superantigen-mediated CD4+, but not CD8+, T-cell expansion. These findings demonstrate that FasL engagement regulates cell-cycle progression, and show that FasL engagement in vivo has a potent anti-inflammatory effect specific for CD4+ T cells.
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页码:1377 / 1382
页数:5
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