Frontiers in Oncology (Jan 2024)

T-cell receptor determinants of response to chemoradiation in locally-advanced HPV16-driven malignancies

  • Pablo Nenclares,
  • Pablo Nenclares,
  • Adrian Larkeryd,
  • Floriana Manodoro,
  • Jen Y. Lee,
  • Susan Lalondrelle,
  • Duncan C. Gilbert,
  • Marco Punta,
  • Ben O’Leary,
  • Ben O’Leary,
  • Antonio Rullan,
  • Antonio Rullan,
  • Anguraj Sadanandam,
  • Benny Chain,
  • Alan Melcher,
  • Kevin J. Harrington,
  • Kevin J. Harrington,
  • Shreerang A. Bhide,
  • Shreerang A. Bhide

DOI
https://doi.org/10.3389/fonc.2023.1296948
Journal volume & issue
Vol. 13

Abstract

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BackgroundThe effect of chemoradiation on the anti-cancer immune response is being increasingly acknowledged; however, its clinical implications in treatment responses are yet to be fully understood. Human papillomavirus (HPV)-driven malignancies express viral oncogenic proteins which may serve as tumor-specific antigens and represent ideal candidates for monitoring the peripheral T-cell receptor (TCR) changes secondary to chemoradiotherapy (CRT).MethodsWe performed intra-tumoral and pre- and post-treatment peripheral TCR sequencing in a cohort of patients with locally-advanced HPV16-positive cancers treated with CRT. An in silico computational pipeline was used to cluster TCR repertoire based on epitope-specificity and to predict affinity between these clusters and HPV16-derived epitopes.ResultsIntra-tumoral repertoire diversity, intra-tumoral and post-treatment peripheral CDR3β similarity clustering were predictive of response. In responders, CRT triggered an increase peripheral TCR clonality and clonal relatedness. Post-treatment expansion of baseline peripheral dominant TCRs was associated with response. Responders showed more baseline clustered structures of TCRs maintained post-treatment and displayed significantly more maintained clustered structures. When applying clustering by TCR-specificity methods, responders displayed a higher proportion of intra-tumoral TCRs predicted to recognise HPV16 peptides.ConclusionsBaseline TCR characteristics and changes in the peripheral T-cell clones triggered by CRT are associated with treatment outcome. Maintenance and boosting of pre-existing clonotypes are key elements of an effective anti-cancer immune response driven by CRT, supporting a paradigm in which the immune system plays a central role in the success of CRT in current standard-of-care protocols.

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