Nature Communications (Feb 2025)

Vaccine-induced T cell receptor T cell therapy targeting a glioblastoma stemness antigen

  • Yu-Chan Chih,
  • Amelie C. Dietsch,
  • Philipp Koopmann,
  • Xiujian Ma,
  • Dennis A. Agardy,
  • Binghao Zhao,
  • Alice De Roia,
  • Alexandros Kourtesakis,
  • Michael Kilian,
  • Christopher Krämer,
  • Abigail K. Suwala,
  • Miriam Stenzinger,
  • Halvard Boenig,
  • Agnieszka Blum,
  • Victor Murcia Pienkowski,
  • Kuralay Aman,
  • Jonas P. Becker,
  • Henrike Feldmann,
  • Theresa Bunse,
  • Richard Harbottle,
  • Angelika B. Riemer,
  • Hai-Kun Liu,
  • Nima Etminan,
  • Felix Sahm,
  • Miriam Ratliff,
  • Wolfgang Wick,
  • Michael Platten,
  • Edward W. Green,
  • Lukas Bunse

DOI
https://doi.org/10.1038/s41467-025-56547-w
Journal volume & issue
Vol. 16, no. 1
pp. 1 – 16

Abstract

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Abstract T cell receptor-engineered T cells (TCR-T) could be advantageous in glioblastoma by allowing safe and ubiquitous targeting of the glioblastoma-derived peptidome. Protein tyrosine phosphatase receptor type Z1 (PTPRZ1), is a clinically targetable glioblastoma antigen associated with glioblastoma cell stemness. Here, we identify a therapeutic HLA-A*02-restricted PTPRZ1-reactive TCR retrieved from a vaccinated glioblastoma patient. Single-cell sequencing of primary brain tumors shows PTPRZ1 overexpression in malignant cells, especially in glioblastoma stem cells (GSCs) and astrocyte-like cells. The validated vaccine-induced TCR recognizes the endogenously processed antigen without off-target cross-reactivity. PTPRZ1-specific TCR-T (PTPRZ1-TCR-T) kill target cells antigen-specifically, and in murine experimental brain tumors, their combined intravenous and intracerebroventricular administration is efficacious. PTPRZ1-TCR-T maintain stem cell memory phenotype in vitro and in vivo and lyse all examined HLA-A*02+ primary glioblastoma cell lines with a preference for GSCs and astrocyte-like cells. In summary, we demonstrate the proof of principle to employ TCR-T to treat glioblastoma.