论文信息 - Functional role of T-cell receptor nanoclusters in signal initiation and antigen discrimination - 字舞流文

Functional role of T-cell receptor nanoclusters in signal initiation and antigen discrimination

Significance T-cell activation requires the translation of antigen binding to the T-cell receptor (TCR) into intracellular signaling. However, how antigen recognition and signal transduction are mechanistically linked is poorly understood. Here, we used single-molecule localization microscopy to link TCR clustering to signaling. We found that the likelihood of a single receptor to initiate signaling upon ligand binding depended on receptor-to-receptor spacing, with TCRs in dense clusters having the highest signaling efficiency. This means that antigen recognition must first be translated into a spatial reorganization of receptors into dense, signaling-competent clusters before signaling can begin. Thus, the quality of an antigen in terms of signaling is given by its ability to densely cluster receptors. Antigen recognition by the T-cell receptor (TCR) is a hallmark of the adaptive immune system. When the TCR engages a peptide bound to the restricting major histocompatibility complex molecule (pMHC), it transmits a signal via the associated CD3 complex. How the extracellular antigen recognition event leads to intracellular phosphorylation remains unclear. Here, we used single-molecule localization microscopy to quantify the organization of TCR–CD3 complexes into nanoscale clusters and to distinguish between triggered and nontriggered TCR–CD3 complexes. We found that only TCR–CD3 complexes in dense clusters were phosphorylated and associated with downstream signaling proteins, demonstrating that the molecular density within clusters dictates signal initiation. Moreover, both pMHC dose and TCR–pMHC affinity determined the density of TCR–CD3 clusters, which scaled with overall phosphorylation levels. Thus, TCR–CD3 clustering translates antigen recognition by the TCR into signal initiation by the CD3 complex, and the formation of dense signaling-competent clusters is a process of antigen discrimination.

Katharina Gaus | Yuanqing Ma | Oreste Acuto | Jamie Rossjohn | Robert G Parton | K. Gaus | A. Sewell | J. Rossjohn | G. Dolton | Yuanqing Ma | P. Nicovich | Yui Yamamoto | Sophie V. Pageon | Jérémie Rossy | R. Parton | J. Gooding | T. Tabarin | O. Acuto | Andrew K Sewell | David A Price | Garry Dolton | J. Bridgeman | Sophie V Pageon | Thibault Tabarin | Yui Yamamoto | Philip R Nicovich | John S Bridgeman | André Cohnen | Carola Benzing | Yijun Gao | Michael D Crowther | Katie Tungatt | J Justin Gooding | Jérémie Rossy | D. Price | A. Cohnen | Michael D. Crowther | C. Benzing | Yijun Gao | K. Tungatt | D. Price | M. Crowther

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