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

نویسندگان

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

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.

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عنوان ژورنال:
  • Proceedings of the National Academy of Sciences of the United States of America

دوره 113 37  شماره 

صفحات  -

تاریخ انتشار 2016