Nature Communications (Dec 2024)

High-resolution profile of neoantigen-specific TCR activation links moderate stimulation to increased resilience of engineered TCR-T cells

  • Franziska Füchsl,
  • Johannes Untch,
  • Vladyslav Kavaka,
  • Gabriela Zuleger,
  • Sarah Braun,
  • Antonia Schwanzer,
  • Sebastian Jarosch,
  • Carolin Vogelsang,
  • Niklas de Andrade Krätzig,
  • Dario Gosmann,
  • Rupert Öllinger,
  • Piero Giansanti,
  • Michael Hiltensperger,
  • Roland Rad,
  • Dirk H. Busch,
  • Eduardo Beltrán,
  • Eva Bräunlein,
  • Angela M. Krackhardt

DOI
https://doi.org/10.1038/s41467-024-53911-0
Journal volume & issue
Vol. 15, no. 1
pp. 1 – 19

Abstract

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Abstract Neoantigen-specific T cell receptors (neoTCRs) promise safe, personalized anti-tumor immunotherapy. However, detailed assessment of neoTCR-characteristics affecting therapeutic efficacy is mostly missing. Previously, we identified diverse neoTCRs restricted to different neoantigens in a melanoma patient. In this work, we now combine single-cell TCR-sequencing and RNA-sequencing after neoantigen-specific restimulation of peripheral blood-derived CD8+ T cells of this patient. We detect neoTCRs with specificity for the previously detected neoantigens and perform fine-characterization of neoTCR-transgenic (tg) T cells in vitro and in vivo. We describe a heterogeneous spectrum of TCR-intrinsic activation patterns in response to a shared neoepitope ranging from previously detected more highly frequent neoTCRs with moderate activation to rare ones with initially stronger activation. Experimental restimulation of adoptively transferred neoTCR-tg T cells in a xenogeneic rechallenge tumor model demonstrates superior anti-tumor responses of moderate neoTCR-tg T cells upon repeated tumor contact. These insights have significant implications for the selection of TCRs for therapeutic engineering of TCR-tg T cells.