OncoImmunology (Apr 2018)

Dynamic changes of the normal B lymphocyte repertoire in CLL in response to ibrutinib or FCR chemo-immunotherapy

  • Simon Schliffke,
  • Mariela Sivina,
  • Ekaterina Kim,
  • Lisa von Wenserski,
  • Benjamin Thiele,
  • Nuray Akyüz,
  • Clemens Falker-Gieske,
  • Donjete Statovci,
  • Anna Oberle,
  • Toni Thenhausen,
  • Artus Krohn-Grimberghe,
  • Carsten Bokemeyer,
  • Nitin Jain,
  • Zeev Estrov,
  • Alessandra Ferrajoli,
  • William Wierda,
  • Michael Keating,
  • Jan A. Burger,
  • Mascha Binder

DOI
https://doi.org/10.1080/2162402X.2017.1417720
Journal volume & issue
Vol. 7, no. 4

Abstract

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Using next-generation immunoglobulin (IGH) sequencing and flow cytometry, we characterized the composition, diversity and dynamics of non-malignant B cells in patients undergoing treatment with the Bruton tyrosine kinase (BTK) inhibitor ibrutinib or chemo-immunotherapy with fludarabine, cyclophosphamide, and rituximab (FCR). During ibrutinib therapy, non-malignant B cell numbers declined, but patients maintained stable IGH diversity and constant fractions of IGH-mutated B cells. This indicates partial preservation of antigen-experienced B cells during ibrutinib therapy, but impaired replenishment of the normal B cell pool with naïve B cells. In contrast, after FCR we noted a recovery of normal B cells with a marked predominance of B cells with unmutated IGH. This pattern is compatible with a deletion of pre-existing antigen-experienced B cells followed by repertoire renewal with antigen-naïve B cells. These opposite patterns in B cell dynamics may result in different responses towards neoantigens versus recall antigens, which need to be further defined.

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