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Journal ArticleDOI

CD3 gamma contains a phosphoserine-dependent di-leucine motif involved in down-regulation of the T cell receptor.

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TLDR
A general model for intracellular sorting of receptors containing di‐leucine‐ or tyrosine‐based motifs is proposed after incubation of T cells in hypertonic medium severely inhibited PKC‐mediated TCR down‐regulation in non‐mutated T cells, indicating that the TCR was down‐regulated by endocytosis via clathrin coated pits.
Abstract
Several cell surface receptors including the T cell receptor (TCR) are phosphorylated and down-regulated following activation of protein kinase C (PKC). Among other substrates the activated PKC in T cells phosphorylates the CD3 gamma subunit of the TCR. To investigate the role of CD3 gamma phosphorylation in PKC-mediated TCR down-regulation, point mutated CD3 gamma cDNA was transfected into the CD3 gamma-negative T cell line JGN and CD3 gamma transfectants were analysed. Phosphorylation at S126 but not S123 in the cytoplasmic tail of CD3 gamma was required for PKC-mediated down-regulation of the TCR. Furthermore, analysis of a series of CD3 gamma truncation mutants indicated that in addition to S126 phosphorylation a motif C-terminal of S126 was required for TCR down-regulation. Point mutation analyses confirmed this observation and demonstrated that a membrane-proximal di-leucine motif (L131 and L132) in the cytoplasmic tail of CD3 gamma was required for PKC-mediated TCR down-regulation in addition to phosphorylation at S126. Incubation of T cells in hypertonic medium known to disrupt normal clathrin lattices severely inhibited PKC-mediated TCR down-regulation in non-mutated T cells, indicating that the TCR was down-regulated by endocytosis via clathrin coated pits. Based on the present results and previously published observations on intracellular receptor sorting, a general model for intracellular sorting of receptors containing di-leucine- or tyrosine-based motifs is proposed.

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Journal ArticleDOI

Signals for Sorting of Transmembrane Proteins to Endosomes and Lysosomes

TL;DR: This work has shown that peptide motifs serve as a signal for sorting at various stages of the endosomal-lysosomal system and several proteins, including clathrin, AP-2, and Dab2, have been proposed to function as recognition proteins for NPXY signals.
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Serial triggering of many T-cell receptors by a few peptide–MHC complexes

TL;DR: It is shown that a small number of peptide–MHC complexes can achieve a high TCR occupancy, because a single complex can serially engage and trigger up to ∼200 TCRs.
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Association of DAP12 with Activating CD94/NKG2C NK Cell Receptors

TL;DR: The results provide a molecular basis for the assembly of NK cell receptors for MHC class I involved in cellular activation and inhibition.
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Phorbol Esters and SDF-1 Induce Rapid Endocytosis and Down Modulation of the Chemokine Receptor CXCR4

TL;DR: It is indicated that endocytosis can regulate the cell-surface expression of CXCR4 and that SDF-1–mediated down regulation of cell- surface coreceptor expression contributes to chemokine-mediated inhibition of HIV infection.
Journal ArticleDOI

On the dynamics of TCR:CD3 complex cell surface expression and downmodulation.

TL;DR: It is demonstrated that ligation induces TCR downmodulation by preventing recycling rather than inducing internalization, which is mediated by the intracellular retention of ligated complexes and degradation by lysosomes and proteasomes.
References
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Journal ArticleDOI

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Journal ArticleDOI

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Journal ArticleDOI

The Molecular Cell Biology of Interferon-gamma and its Receptor

TL;DR: This review focuses on the new developments in the areas of IFN gamma biochemistry and biology and pays particular attention to the IFN Gamma receptor and three aspects of IFn gamma biology that are of special interest to immunologists: host defense, inflammation, and autoimmunity.
Journal ArticleDOI

NPXY, a sequence often found in cytoplasmic tails, is required for coated pit-mediated internalization of the low density lipoprotein receptor.

TL;DR: A review of published data revealed NPXY sequences in cytoplasmic domains of at least 10 other cell surface proteins, including tyrosine kinase-linked receptors of the epidermal growth factor and insulin receptor family, the beta-subunits of three integrin receptors, and the amyloid A4 precursor protein.
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