Frontiers in Immunology (Jul 2022)

γ9δ2 T-Cell Expansion and Phenotypic Profile Are Reflected in the CDR3δ Repertoire of Healthy Adults

  • Anna Vyborova,
  • Anke Janssen,
  • Lucrezia Gatti,
  • Froso Karaiskaki,
  • Austin Yonika,
  • Sanne van Dooremalen,
  • Jasper Sanders,
  • Dennis X. Beringer,
  • Trudy Straetemans,
  • Trudy Straetemans,
  • Zsolt Sebestyen,
  • Jürgen Kuball,
  • Jürgen Kuball

DOI
https://doi.org/10.3389/fimmu.2022.915366
Journal volume & issue
Vol. 13

Abstract

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γ9δ2T cells fill a distinct niche in human immunity due to the unique physiology of the phosphoantigen-reactive γ9δ2TCR. Here, we highlight reproducible TCRδ complementarity-determining region 3 (CDR3δ) repertoire patterns associated with γ9δ2T cell proliferation and phenotype, thus providing evidence for the role of the CDR3δ in modulating in vivo T-cell responses. Features that determine γ9δ2TCR binding affinity and reactivity to the phosphoantigen-induced ligand in vitro appear to similarly underpin in vivo clonotypic expansion and differentiation. Likewise, we identify a CDR3δ bias in the γ9δ2T cell natural killer receptor (NKR) landscape. While expression of the inhibitory receptor CD94/NKG2A is skewed toward cells bearing putative high-affinity TCRs, the activating receptor NKG2D is expressed independently of the phosphoantigen-sensing determinants, suggesting a higher net NKR activating signal in T cells with TCRs of low affinity. This study establishes consistent repertoire–phenotype associations and justifies stratification for the T-cell phenotype in future research on γ9δ2TCR repertoire dynamics.

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