Cell Reports (Feb 2016)

Diversity of the CD4 T Cell Alloresponse: The Short and the Long of It

  • Jason M. Ali,
  • Margaret C. Negus,
  • Thomas M. Conlon,
  • Ines G. Harper,
  • M. Saeed Qureshi,
  • Reza Motallebzadeh,
  • Richard Willis,
  • Kourosh Saeb-Parsy,
  • Eleanor M. Bolton,
  • J. Andrew Bradley,
  • Gavin J. Pettigrew

Journal volume & issue
Vol. 14, no. 5
pp. 1232 – 1245

Abstract

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Summary: MHC alloantigen is recognized by two pathways: “directly,” intact on donor cells, or “indirectly,” as self-restricted allopeptide. The duration of each pathway, and its relative contribution to allograft vasculopathy, remain unclear. Using a murine model of chronic allograft rejection, we report that direct-pathway CD4 T cell alloresponses, as well as indirect-pathway responses against MHC class II alloantigen, are curtailed by rapid elimination of donor hematopoietic antigen-presenting cells. In contrast, persistent presentation of epitope resulted in continual division and less-profound contraction of the class I allopeptide-specific CD4 T cell population, with approximately 10,000-fold more cells persisting than following acute allograft rejection. This expanded population nevertheless displayed sub-optimal anamnestic responses and was unable to provide co-stimulation-independent help for generating alloantibody. Indirect-pathway CD4 T cell responses are heterogeneous. Appreciation that responses against particular alloantigens dominate at late time points will likely inform development of strategies aimed at improving transplant outcomes. : The T cell allorecognition pathways governing rejection of organ allografts are poorly understood. Using a model of chronic heart graft rejection, Ali et al. show that continual presentation of MHC class I allopeptide drives late division in the responding alloreactive CD4 T cell population, resulting in a markedly augmented maintenance phase.