Depletion of the programmed death-1 receptor completely reverses established clonal anergy in CD4(+) T lymphocytes via an interleukin-2-dependent mechanism
Bishop, Kenneth D. ; Harris, John E. ; Mordes, John P. ; Greiner, Dale L. ; Rossini, Aldo A. ; Czech, Michael P. ; Phillips, Nancy E.
Bishop, Kenneth D.
Harris, John E.
Mordes, John P.
Greiner, Dale L.
Rossini, Aldo A.
Czech, Michael P.
Phillips, Nancy E.
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Journal Article
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2009-02-24
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Abstract
Recent studies have implicated the cell surface receptor Programmed Death-1 (PD-1) in numerous models of T cell anergy, though the specific mechanisms by which the PD-1 signal maintains tolerance is not clear. We demonstrate that the depletion of PD-1 with siRNA results in a complete reversal of clonal anergy in the A.E7 T cell model, suggesting that the mechanism by which PD-1 maintains the anergic phenotype is a T-cell-intrinsic phenomenon, and not one dependent on other cell populations in vivo. We have also shown that the neutralization of IL-2 during restimulation abrogates the effect of PD-1 depletion, suggesting that tolerance mediated by PD-1 is wholly IL-2 dependent, and likewise intrinsic to the tolerized cells.
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19230866
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Citation: Cell Immunol. 2009;256(1-2):86-91. Epub 2009 Feb 23. <a href="http://dx.doi.org/10.1016/j.cellimm.2009.01.008">Link to article on publisher's site</a>