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The Affinity of Elongated Membrane-Tethered Ligands Determines Potency of T Cell Receptor Triggering.


ABSTRACT: T lymphocytes are important mediators of adoptive immunity but the mechanism of T cell receptor (TCR) triggering remains uncertain. The interspatial distance between engaged T cells and antigen-presenting cells (APCs) is believed to be important for topological rearrangement of membrane tyrosine phosphatases and initiation of TCR signaling. We investigated the relationship between ligand topology and affinity by generating a series of artificial APCs that express membrane-tethered anti-CD3 scFv with different affinities (OKT3, BC3, and 2C11) in addition to recombinant class I and II pMHC molecules. The dimensions of membrane-tethered anti-CD3 and pMHC molecules were progressively increased by insertion of different extracellular domains. In agreement with previous studies, elongation of pMHC molecules or low-affinity anti-CD3 scFv caused progressive loss of T cell activation. However, elongation of high-affinity ligands (BC3 and OKT3 scFv) did not abolish TCR phosphorylation and T cell activation. Mutation of key amino acids in OKT3 to reduce binding affinity to CD3 resulted in restoration of topological dependence on T cell activation. Our results show that high-affinity TCR ligands can effectively induce TCR triggering even at large interspatial distances between T cells and APCs.

SUBMITTER: Chen BM 

PROVIDER: S-EPMC5502409 | biostudies-literature | 2017

REPOSITORIES: biostudies-literature

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The Affinity of Elongated Membrane-Tethered Ligands Determines Potency of T Cell Receptor Triggering.

Chen Bing-Mae BM   Al-Aghbar Mohammad Ameen MA   Lee Chien-Hsin CH   Chang Tien-Ching TC   Su Yu-Cheng YC   Li Ya-Chen YC   Chang Shih-En SE   Chen Chin-Chuan CC   Chung Tsai-Hua TH   Liao Yuan-Chun YC   Lee Chau-Hwang CH   Roffler Steve R SR  

Frontiers in immunology 20170710


T lymphocytes are important mediators of adoptive immunity but the mechanism of T cell receptor (TCR) triggering remains uncertain. The interspatial distance between engaged T cells and antigen-presenting cells (APCs) is believed to be important for topological rearrangement of membrane tyrosine phosphatases and initiation of TCR signaling. We investigated the relationship between ligand topology and affinity by generating a series of artificial APCs that express membrane-tethered anti-CD3 scFv  ...[more]

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