OncoImmunology (Jun 2018)

Restricted T cell receptor repertoire in CLL-like monoclonal B cell lymphocytosis and early stage CLL

  • Gonzalo Blanco,
  • Anna Vardi,
  • Anna Puiggros,
  • Andrea Gómez-Llonín,
  • Manuel Muro,
  • María Rodríguez-Rivera,
  • Evangelia Stalika,
  • Eugenia Abella,
  • Eva Gimeno,
  • Manuela López-Sánchez,
  • Alicia Senín,
  • Xavier Calvo,
  • Pau Abrisqueta,
  • Francesc Bosch,
  • Ana Ferrer,
  • Kostas Stamatopoulos,
  • Blanca Espinet

DOI
https://doi.org/10.1080/2162402X.2018.1432328
Journal volume & issue
Vol. 7, no. 6

Abstract

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Analysis of the T cell receptor (TR) repertoire of chronic lymphocytic leukemia-like monoclonal B cell lymphocytosis (CLL-like MBL) and early stage CLL is relevant for understanding the dynamic interaction of expanded B cell clones with bystander T cells. Here we profiled the T cell receptor β chain (TRB) repertoire of the CD4+ and CD8+ T cell fractions from 16 CLL-like MBL and 13 untreated, Binet stage A/Rai stage 0 CLL patients using subcloning analysis followed by Sanger sequencing. The T cell subpopulations of both MBL and early stage CLL harbored restricted TRB gene repertoire, with CD4+ T cell clonal expansions whose frequency followed the numerical increase of clonal B cells. Longitudinal analysis in MBL cases revealed clonal persistence, alluding to persistent antigen stimulation. In addition, the identification of shared clonotypes among different MBL/early stage CLL cases pointed towards selection of the T cell clones by common antigenic elements. T cell clonotypes previously described in viral infections and immune disorders were also detected. Altogether, our findings evidence that antigen-mediated TR restriction occurs early in clonal evolution leading to CLL and may further increase together with B cell clonal expansion, possibly suggesting that the T cell selecting antigens are tumor-related.

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