Journal for ImmunoTherapy of Cancer (Oct 2023)

Neoantigen-specific CD4+ tumor-infiltrating lymphocytes are potent effectors identified within adoptive cell therapy products for metastatic melanoma patients

  • Shari Pilon-Thomas,
  • Daniel Abate-Daga,
  • Amod A. Sarnaik,
  • James J. Mule,
  • Xiaoqing Yu,
  • Patrick Innamarato,
  • Jamie Blauvelt,
  • Holly Branthoover,
  • Jake Ceccarelli,
  • TJ Langer,
  • MacLean S. Hall,
  • Jamie K. Teer,
  • Sebastian Snedal,
  • Madeline Rodriguez-Valentin,
  • Luz Nagle,
  • Ellen Scott,
  • Ben Schachner,
  • Amy M. Hall,
  • Carolyn J. Rich,
  • Allison D. Richards,
  • Sean J. Yoder,
  • Matthew S. Beatty,
  • Cheryl A. Cox,
  • Jane L. Messina,
  • John E. Mullinax

DOI
https://doi.org/10.1136/jitc-2023-007288
Journal volume & issue
Vol. 11, no. 10

Abstract

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Background Adoptive cell therapy (ACT) with tumor-infiltrating lymphocytes (TILs) is a promising immunotherapeutic approach for patients with advanced solid tumors. While numerous advances have been made, the contribution of neoantigen-specific CD4+T cells within TIL infusion products remains underexplored and therefore offers a significant opportunity for progress.Methods We analyzed infused TIL products from metastatic melanoma patients previously treated with ACT for the presence of neoantigen-specific T cells. TILs were enriched on reactivity to neoantigen peptides derived and prioritized from patient sample-directed mutanome analysis. Enriched TILs were further investigated to establish the clonal neoantigen response with respect to function, transcriptomics, and persistence following ACT.Results We discovered that neoantigen-specific TIL clones were predominantly CD4+ T cells and were present in both therapeutic responders and non-responders. CD4+ TIL demonstrated an effector T cell response with cytotoxicity toward autologous tumor in a major histocompatibility complex class II-dependent manner. These results were validated by paired TCR and single cell RNA sequencing, which elucidated transcriptomic profiles distinct to neoantigen-specific CD4+ TIL.Conclusions Despite methods which often focus on CD8+T cells, our study supports the importance of prospective identification of neoantigen-specific CD4+ T cells within TIL products as they are a potent source of tumor-specific effectors. We further advocate for the inclusion of neoantigen-specific CD4+ TIL in future ACT protocols as a strategy to improve antitumor immunity.