Literature DB >> 24860189

TCR Microclusters pre-exist and contain molecules necessary for TCR signal transduction.

Travis J Crites1, Kartika Padhan1, James Muller2, Michelle Krogsgaard3, Prabhakar R Gudla4, Stephen J Lockett4, Rajat Varma5.   

Abstract

TCR-dependent signaling events have been observed to occur in TCR microclusters. We found that some TCR microclusters are present in unstimulated murine T cells, indicating that the mechanisms leading to microcluster formation do not require ligand binding. These pre-existing microclusters increase in absolute number following engagement by low-potency ligands. This increase is accompanied by an increase in cell spreading, with the result that the density of TCR microclusters on the surface of the T cell is not a strong function of ligand potency. In characterizing their composition, we observed a constant number of TCRs in a microcluster, constitutive exclusion of the phosphatase CD45, and preassociation with the signaling adapters linker for activation of T cells and growth factor receptor-bound protein 2. The existence of TCR microclusters prior to ligand binding in a state that is conducive for the initiation of downstream signaling could explain, in part, the rapid kinetics with which TCR signal transduction occurs.

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Year:  2014        PMID: 24860189      PMCID: PMC4096552          DOI: 10.4049/jimmunol.1400315

Source DB:  PubMed          Journal:  J Immunol        ISSN: 0022-1767            Impact factor:   5.422


  41 in total

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Authors:  Rajat Varma; Gabriele Campi; Tadashi Yokosuka; Takashi Saito; Michael L Dustin
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  23 in total

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5.  The cellular environment regulates in situ kinetics of T-cell receptor interaction with peptide major histocompatibility complex.

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6.  Lattice Light-Sheet Microscopy Multi-dimensional Analyses (LaMDA) of T-Cell Receptor Dynamics Predict T-Cell Signaling States.

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7.  Tetraspanin-5-mediated MHC class I clustering is required for optimal CD8 T cell activation.

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