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Review
. 2007 Jun;19(3):153-61.
doi: 10.1016/j.smim.2007.02.007. Epub 2007 Mar 26.

Molecular basis for checkpoints in the CD8 T cell response: tolerance versus activation

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Review

Molecular basis for checkpoints in the CD8 T cell response: tolerance versus activation

Matthew F Mescher et al. Semin Immunol. 2007 Jun.

Abstract

CD8 T cells specific for self-antigens are present in the peripheral lymphoid system and can contribute to autoimmunity or transplant rejection. Whether recognition of Ag leads to full activation, or to induction of tolerance, depends upon availability of cytokine at critical stages of the response. Signals provided by IL-12 and/or IFN-alpha/beta are required for activation of naïve CD8 T cells, and IL-2 is needed to sustain and further expand the effector cells if Ag persists. These critical signaling requirements provide new insights into the factors that regulate the CD8 T cell contributions to development of autoimmunity or rejection of transplants.

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Figures

Figure 1
Figure 1
MAP kinase activation in naïve and effector (AINR) CD8 T cell, and cells that have been stimulated with IL-2 to reverse AINR. Cells were stimulated with either Ag (TCR) or Ag and B7-1 (TCR/CD28) and kinase activity measured for ERK and JNK, and phosphorylation measured for p38 [51]. Shaded regions highlight the ‘re-wiring’ that occurs upon reversal of AINR.
Figure 2
Figure 2
CD8 T cells require cytokine signaling to traverse checkpoints in the response and avoid tolerance.

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