Frontiers in Immunology (Oct 2021)

Non-Stimulatory pMHC Enhance CD8 T Cell Effector Functions by Recruiting Coreceptor-Bound Lck

  • Xiang Zhao,
  • Xiang Zhao,
  • Liang-Zhe Wu,
  • Liang-Zhe Wu,
  • Esther K. Y. Ng,
  • Esther K. Y. Ng,
  • Kerisa W. S. Leow,
  • Qianru Wei,
  • Qianru Wei,
  • Nicholas R. J. Gascoigne,
  • Nicholas R. J. Gascoigne,
  • Joanna Brzostek,
  • Joanna Brzostek

DOI
https://doi.org/10.3389/fimmu.2021.721722
Journal volume & issue
Vol. 12

Abstract

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Under physiological conditions, CD8+ T cells need to recognize low numbers of antigenic pMHC class I complexes in the presence of a surplus of non-stimulatory, self pMHC class I on the surface of the APC. Non-stimulatory pMHC have been shown to enhance CD8+ T cell responses to low amounts of antigenic pMHC, in a phenomenon called co-agonism, but the physiological significance and molecular mechanism of this phenomenon are still poorly understood. Our data show that co-agonist pMHC class I complexes recruit CD8-bound Lck to the immune synapse to modulate CD8+ T cell signaling pathways, resulting in enhanced CD8+ T cell effector functions and proliferation, both in vitro and in vivo. Moreover, co-agonism can boost T cell proliferation through an extrinsic mechanism, with co-agonism primed CD8+ T cells enhancing Akt pathway activation and proliferation in neighboring CD8+ T cells primed with low amounts of antigen.

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