Molecular Therapy: Oncolytics (Mar 2023)

A library of cancer testis specific T cell receptors for T cell receptor gene therapy

  • Marije A.J. de Rooij,
  • Dennis F.G. Remst,
  • Dirk M. van der Steen,
  • Anne K. Wouters,
  • Renate S. Hagedoorn,
  • Michel G.D. Kester,
  • Miranda H. Meeuwsen,
  • Tassilo L.A. Wachsmann,
  • Arnoud H. de Ru,
  • Peter A. van Veelen,
  • Els M.E. Verdegaal,
  • J.H. Frederik Falkenburg,
  • Mirjam H.M. Heemskerk

Journal volume & issue
Vol. 28
pp. 1 – 14

Abstract

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To increase the number of cancer patients that can be treated with T cell receptor (TCR) gene therapy, we aimed to identify a set of high-affinity cancer-specific TCRs targeting different melanoma-associated antigens (MAGEs). In this study, peptides derived from MAGE genes with tumor-specific expression pattern were identified by human leukocyte antigen (HLA) peptidomics. Next, peptide-HLA tetramers were generated, and used to sort MAGE-specific CD8+ T cell clones from the allogeneic (allo) HLA repertoire of healthy donors. To evaluate the clinical potential, most potent TCRs were sequenced, transferred into peripheral blood-derived CD8+ T cells, and tested for antitumor efficacy. In total we identified, seven MAGE-specific TCRs that effectively target MAGE-A1, MAGE-A3, MAGE-A6, and MAGE-A9 in the context of HLA-A∗01:01, -A∗02:01, -A∗03:01, -B∗07:02, -B∗35:01, or -C∗07:02. TCR gene transfer into CD8⁺ T cells resulted in efficient reactivity against a variety of different tumor types, while no cross-reactivity was detected. In addition, major in vivo antitumor effects of MAGE-A1 specific TCR engineered CD8⁺ T cells were observed in the orthotopic xenograft model for established multiple myeloma. The identification of seven MAGE-specific TCRs expands the pool of cancer patients eligible for TCR gene therapy and increases possibilities for personalized TCR gene therapy.

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