Journal of Hematology & Oncology (Feb 2023)

Broadly applicable TCR-based therapy for multiple myeloma targeting the immunoglobulin J chain

  • Miranda H. Meeuwsen,
  • Anne K. Wouters,
  • Tassilo L. A. Wachsmann,
  • Renate S. Hagedoorn,
  • Michel G. D. Kester,
  • Dennis F. G. Remst,
  • Dirk M. van der Steen,
  • Arnoud H. de Ru,
  • Els P. van Hees,
  • Martijn Kremer,
  • Marieke Griffioen,
  • Peter A. van Veelen,
  • J. H. Frederik Falkenburg,
  • Mirjam H. M. Heemskerk

DOI
https://doi.org/10.1186/s13045-023-01408-6
Journal volume & issue
Vol. 16, no. 1
pp. 1 – 16

Abstract

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Abstract Background The immunoglobulin J chain (Jchain) is highly expressed in the majority of multiple myeloma (MM), and Jchain-derived peptides presented in HLA molecules may be suitable antigens for T-cell therapy of MM. Methods Using immunopeptidomics, we identified Jchain-derived epitopes presented by MM cells, and pHLA tetramer technology was used to isolate Jchain-specific T-cell clones. Results We identified T cells specific for Jchain peptides presented in HLA-A1, -A24, -A3, and -A11 that recognized and lysed JCHAIN-positive MM cells. TCRs of the most promising T-cell clones were sequenced, cloned into retroviral vectors, and transferred to CD8 T cells. Jchain TCR T cells recognized target cells when JCHAIN and the appropriate HLA restriction alleles were expressed, while JCHAIN or HLA-negative cells, including healthy subsets, were not recognized. Patient-derived JCHAIN-positive MM samples were also lysed by Jchain TCR T cells. In a preclinical in vivo model for established MM, Jchain-A1, -A24, -A3, and -A11 TCR T cells strongly eradicated MM cells, which resulted in 100-fold lower tumor burden in Jchain TCR versus control-treated mice. Conclusions We identified TCRs targeting Jchain-derived peptides presented in four common HLA alleles. All four TCRs demonstrated potent preclinical anti-myeloma activity, encouraging further preclinical testing and ultimately clinical development.