2012
DOI: 10.1073/pnas.1217409110
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Distinct mechanisms mediate naïve and memory CD8 T-cell tolerance

Abstract: Peripheral tolerance to developmentally regulated antigens is necessary to sustain tissue homeostasis. We have now devised an inducible and reversible system that allows interrogation of T-cell tolerance induction in endogenous naïve and memory CD8 T cells. Our data show that peripheral CD8 T-cell tolerance can be preserved through two distinct mechanisms, antigen addiction leading to anergy for naïve T cells and ignorance for memory T cells. Induction of antigen in dendritic cells resulted in substantial expa… Show more

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Cited by 14 publications
(14 citation statements)
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“…These observations are consistent with the hypothesis that the increased sensitivity of memory T cells to elaborate effector function has to be balanced with tight control in order to limit their pathogenicity. Increased antigen threshold requirements have been reported for memory CD4 + and CD8 + T cells, resulting in preferential proliferation of naive T cells over memory cells (46)(47)(48)(49)(50). Thus, it is possible that the proliferation observed in our presensitized mice following B/c heart transplantation was actually driven predominantly by naive cells rather than by memory T cells, thereby explaining our observation that CTLA4-Ig inhibited donor-specific T cell expansion in sensitized recipients.…”
Section: Cd4mentioning
confidence: 35%
“…These observations are consistent with the hypothesis that the increased sensitivity of memory T cells to elaborate effector function has to be balanced with tight control in order to limit their pathogenicity. Increased antigen threshold requirements have been reported for memory CD4 + and CD8 + T cells, resulting in preferential proliferation of naive T cells over memory cells (46)(47)(48)(49)(50). Thus, it is possible that the proliferation observed in our presensitized mice following B/c heart transplantation was actually driven predominantly by naive cells rather than by memory T cells, thereby explaining our observation that CTLA4-Ig inhibited donor-specific T cell expansion in sensitized recipients.…”
Section: Cd4mentioning
confidence: 35%
“…S1e ). KLRG1 expression, related to terminally differentiated CD8+ T cells and senescence 22 23 , and expression of CD127 (IL-7R), which is associated with memory phenotypes and downregulation of which has been linked to deletional tolerance, were also measured 21 . Expression of both CD127 and KLRG1 were significantly lower in response to erythrocyte-targeted versus soluble antigens ( Fig.…”
Section: Resultsmentioning
confidence: 99%
“…It would be interesting to know whether reduced sensitivity to TCR signaling promotes the expression of Egr2 and GRAIL. Memory CD8 + T cells are susceptible to peripheral tolerance (Kreuwel et al, 2002;Jellison et al, 2012), though memory T cell responses are resistant to co-stimulation blockade and anti-TCR mAb treatment (Miyahara et al, 2012). Defining the role of Egr2, GRAIL, and many other intracellular regulators in memory T cell responses is critical for inducing transplant tolerance and preventing autoimmunity.…”
Section: Discussionmentioning
confidence: 99%