PLoS ONE (Jan 2015)

Somatic Variation of T-Cell Receptor Genes Strongly Associate with HLA Class Restriction.

  • Paul L Klarenbeek,
  • Marieke E Doorenspleet,
  • Rebecca E E Esveldt,
  • Barbera D C van Schaik,
  • Neubury Lardy,
  • Antoine H C van Kampen,
  • Paul P Tak,
  • Robert M Plenge,
  • Frank Baas,
  • Paul I W de Bakker,
  • Niek de Vries

DOI
https://doi.org/10.1371/journal.pone.0140815
Journal volume & issue
Vol. 10, no. 10
p. e0140815

Abstract

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Every person carries a vast repertoire of CD4+ T-helper cells and CD8+ cytotoxic T cells for a healthy immune system. Somatic VDJ recombination at genomic loci that encode the T-cell receptor (TCR) is a key step during T-cell development, but how a single T cell commits to become either CD4+ or CD8+ is poorly understood. To evaluate the influence of TCR sequence variation on CD4+/CD8+ lineage commitment, we sequenced rearranged TCRs for both α and β chains in naïve T cells isolated from healthy donors and investigated gene segment usage and recombination patterns in CD4+ and CD8+ T-cell subsets. Our data demonstrate that most V and J gene segments are strongly biased in the naïve CD4+ and CD8+ subsets with some segments increasing the odds of being CD4+ (or CD8+) up to five-fold. These V and J gene associations are highly reproducible across individuals and independent of classical HLA genotype, explaining ~11% of the observed variance in the CD4+ vs. CD8+ propensity. In addition, we identified a strong independent association of the electrostatic charge of the complementarity determining region 3 (CDR3) in both α and β chains, where a positively charged CDR3 is associated with CD4+ lineage and a negatively charged CDR3 with CD8+ lineage. Our findings suggest that somatic variation in different parts of the TCR influences T-cell lineage commitment in a predominantly additive fashion. This notion can help delineate how certain structural features of the TCR-peptide-HLA complex influence thymic selection.