OncoImmunology (Feb 2018)

The inhibitory checkpoint, PD-L2, is a target for effector T cells: Novel possibilities for immune therapy

  • Shamaila Munir Ahmad,
  • Evelina Martinenaite,
  • Morten Holmström,
  • Mia Aaboe Jørgensen,
  • Özcan Met,
  • Claudia Nastasi,
  • Uffe Klausen,
  • Marco Donia,
  • Lars Møller Pedersen,
  • Lars Munksgaard,
  • Niels Ødum,
  • Anders Woetmann,
  • Inge Marie Svane,
  • Mads Hald Andersen

DOI
https://doi.org/10.1080/2162402X.2017.1390641
Journal volume & issue
Vol. 7, no. 2

Abstract

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Cell surface molecules of the B7/CD28 family play an important role in T-cell activation and tolerance. The relevance of the PD-1/PD-L1 pathway in cancer has been extensively studied whereas PD-L2 has received less attention. However, recently the expression of PD-L2 was described to be independently associated with clinical response in anti-PD1-treated cancer patients. Here, we investigated whether PD-L2 might represent a natural target that induces specific T cells. We identified spontaneous specific T-cell reactivity against two epitopes located in the signal peptide of PD-L2 from samples from patients with cancer as well as healthy individuals ex vivo. We characterized both CD8+ and CD4+ PD-L2-specific T cells. Interestingly, the epitope in PD-L2 that elicited the strongest response was equivalent to a potent HLA-A2-restricted epitope in PD-L1. Importantly, PD-L1-specific and PD-L2-specific T cells did not cross-react; therefore, they represent different T-cell antigens. Moreover, PD-L2-specific T cells reacted to autologous target cells depending on PD-L2 expression. These results suggested that activating PD-L2 specific T cells (e.g., by vaccination) might be an attractive strategy for anti-cancer immunotherapy. Accordingly, PD-L2 specific T cells can directly support anti-cancer immunity by killing of target cells, as well as, indirectly, by releasing pro-inflammatory cytokines at the microenvironment in response to PD-L2-expressing immune supressive cells.

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