Frontiers in Immunology (Aug 2023)

Analysis of tumor infiltrating CD4+ and CD8+ CDR3 sequences reveals shared features putatively associated to the anti-tumor immune response

  • Andrea Aran,
  • Gonzalo Lázaro,
  • Vicente Marco,
  • Elisa Molina,
  • Ferran Abancó,
  • Vicente Peg,
  • Vicente Peg,
  • Vicente Peg,
  • María Gión,
  • Laia Garrigós,
  • José Pérez-García,
  • José Pérez-García,
  • Javier Cortés,
  • Javier Cortés,
  • Javier Cortés,
  • Mercè Martí,
  • Mercè Martí

DOI
https://doi.org/10.3389/fimmu.2023.1227766
Journal volume & issue
Vol. 14

Abstract

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IntroductionTumor-infiltrating lymphocytes (TILs) have predictive and prognostic value in breast cancer (BC) and exert a protective function against tumor growth, indicating that it is susceptible to treatment using adoptive cell transfer of TILs or T cell receptor (TCR)-based therapies. TCR can be used to identify naturally tumor-reactive T cells, but little is known about the differences in the TCR repertoires of CD4+ and CD8+ TILs.MethodsTCR high-throughput sequencing was performed using TILs derived from the initial cultures of 11 BC biopsies and expanded and sorted CD4+ and CD8+ TILs as well as using PBMCs from healthy donors expanded and sorted using the same methodology.ResultsPhysicochemical TCR differences between T cell subsets were observed, as CD4+ TILs presented larger N(D)Nnt TRB sequences and with a higher usage of positively charged residues, although only the latest was also observed in peripheral T cells from healthy individuals. Moreover, in CD4+ TILs, a more restricted TCR repertoire with a higher abundance of similar sequences containing certain amino acid motifs was observed.DiscussionSome differences between CD4+ and CD8+ TCRs were intrinsic to T cell subsets as can also be observed in peripheral T cells from healthy individuals, while other were only found in TILs samples and therefore may be tumor-driven. Notably, the higher similarity among CD4+ TCRs suggests a higher TCR promiscuity in this subset.

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