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Journal ArticleDOI

Developmental regulation of TCR efficiency.

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TLDR
An unexpected characteristic of the T cell receptor is revealed: its ability to signal fully is regulated inversely by its level of expression, which may apply to other receptors both within and outside the immune system.
Abstract
Unresponsiveness of mature T cells to the same self-peptide/self-MHC molecule complexes with which thymocytes have reacted during positive selection results from an increase of activation thresholds during maturation. The molecular events accounting for this increase are still unknown. In mature cells, a strong correlation between the extent of TCR down-modulation and T cell responses has been demonstrated. Exploiting this relationship, we show that the efficiency with which the TCR mediates full signaling is developmentally regulated. It decreases with thymic maturation and then increases with differentiation of naive T cells into memory lymphocytes. This analysis based on TCR modulation revealed an unexpected characteristic of the T cell receptor: its ability to signal fully is regulated inversely by its level of expression. This latter relationship may apply to other receptors both within and outside the immune system.

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Journal ArticleDOI

Positive and Negative Selection of T Cells

TL;DR: The current state of the field regarding the natural ligands and molecular factors required for positive and negative selection are summarized and a model for how these disparate outcomes can be signaled via the same receptor is discussed.
Journal ArticleDOI

Thymocyte Sensitivity and Supramolecular Activation Cluster Formation Are Developmentally Regulated: A Partial Role for Sialylation

TL;DR: It is shown that desialylation of mature CD8 T cells enhances their sensitivity to low-affinity ligands, although these treatments do not completely recapitulate the dynamic range of immature T cells.
Journal ArticleDOI

A role for CD8 in the developmental tuning of antigen recognition and CD3 conformational change.

TL;DR: It is proposed that CD8 participation in the TCR/pMHC interaction can physically regulate CD3Δc induction by “translating” productive Ag encounter from the T CR to the CD3 complex.
Journal ArticleDOI

Characteristics of TCR/CD3 complex CD3ɛ chains of regulatory CD4+ T (Treg) lymphocytes: role in Treg differentiation in vitro and impact on Treg in vivo

TL;DR: Quantitative and qualitative differences in the TCR/CD3 complex are shown, supporting the hyporesponsive phenotype of Tregs concerning TCR/, and these differences might reconcile avidity and flexible threshold models of TReg differentiation and be used to implement therapeutic approaches involving Treg manipulation.
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