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The Journal of Immunology, 1998, 161: 5855-5861.
Copyright © 1998 by The American Association of Immunologists

Differential Role of CTLA-4 in Regulation of Resting Memory Versus Naive CD4 T Cell Activation1

D. P. Metz*, D. L. Farber{dagger}, T. Taylor* and K. Bottomly2,*

* Immunobiology Section, Yale University School of Medicine, New Haven, CT 06510; {dagger} Department of Microbiology, University of Maryland, College Park, MD 20910

Regulation of peripheral T cell responses is critical for preserving self tolerance. Memory T cells have a lower threshold for activation through the TCR and are thought to be less dependent on costimulation than naive T cells, suggesting a requirement for more stringent regulation of memory T cells. We have recently shown that CD4 engagement apart from the TCR results in the inactivation of memory, but not naive, CD4 T cells. We show here that this inhibition requires ligation of CTLA-4, in that blocking CTLA-4-B7 interactions restores memory CD4 T cell responsiveness. Early signaling through CTLA-4 is possible because resting memory, but not naive, CD4 T cells contain intracellular stores of CTLA-4 that are continuously recycled between the cytoplasm and the cell surface. This mechanism ensures that low intensity TCR engagements, which are thought to be important for peripheral T cell longevity, do not cause memory T cell activation but instead raise their threshold for costimulatory signals. This may give memory T cells an extended lifespan with a reduced risk of inappropriate activation.




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