OncoImmunology (Jan 2018)

T cell inhibitory mechanisms in a model of aggressive Non-Hodgkin's Lymphoma

  • Tamara Hilmenyuk,
  • Carla A. Ruckstuhl,
  • Michael Hayoz,
  • Christian Berchtold,
  • Jean-Marc Nuoffer,
  • Shyam Solanki,
  • Hector C. Keun,
  • Paul A. Beavis,
  • Carsten Riether,
  • Adrian F. Ochsenbein

DOI
https://doi.org/10.1080/2162402X.2017.1365997
Journal volume & issue
Vol. 7, no. 1

Abstract

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A reduced immune surveillance due to immune deficiency or treatment with immunosuppressive drugs is associated with a higher risk to develop aggressive Non-Hodgkin's lymphoma (NHL). Nevertheless, NHL also develops in immunocompetent patients indicating an escape from the immune system. T cell function in advanced aggressive lymphoma is not well characterized and the molecular mechanisms how malignant B cells influence T cell function are ill-defined. We therefore studied T cell function in Eμ-myc transgenic mice that develop an aggressive B cell lymphoma with some similarities to human Burkitt-lymphoma (BL). In advanced lymphoma, the number of T cells was severely reduced and the remaining CD4+ and CD8+ T cells lost the capacity to produce effector cytokines and expand upon re-stimulation. T cells in lymphoma-bearing mice were characterized by the expression of the immune inhibitory molecules programmed death (PD)-1, 2B4 and lymphocyte activation protein (LAG)-3. The proto-oncogene c-Myc not only drives cell proliferation and disease progression but also induces apoptosis of the malignant cells. We found that apoptotic lymphoma cells release purine metabolites that inhibit T cell function. Taken together, our data document that the characteristic high cell turnover and apoptotic rate in aggressive NHL induce a severe T cell dysfunction mediated by several immune-inhibitory mechanisms including ligation of inhibitory ligands and purine metabolites. Blocking a single mechanism only partially restored T cell function and did not increase survival of lymphoma mice.

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