Beneficial role of CD8+ T-cell reconstitution after HLA-haploidentical stem cell transplantation for high-risk acute leukaemias: results from a clinico-biological EBMT registry study mostly in the T-cell-depleted setting

  • Attilio Bondanza
  • , Loredana Ruggeri
  • , Maddalena Noviello
  • , Dirk-Jan Eikema
  • , Chiara Bonini
  • , Christian Chabannon
  • , Steffie Van Der Werf
  • , Anja Van Biezen
  • , Liesbeth C. De Wreede
  • , Lara Crucitti
  • , Luca Vago
  • , Mara Merluzzi
  • , Maria Speranza Massei
  • , Hendrik Veelken
  • , Yener Koc
  • , Peter Bader
  • , Bernd Gruhn
  • , Franco Locatelli
  • , Fabio Ciceri
  • , Antoine Toubert
  • Andrea Velardi

Risultato della ricerca: Contributo in rivistaArticolo

Abstract

HLA-haploidentical haematopoietic stem cell transplantation (haplo-HSCT) is increasingly offered to patients with high-risk acute leukaemia. Unfortunately, haplo-HSCT is followed by a delayed immunoreconstitution. The aim of this EBMT registry study was to explore the clinical impact of lymphocyte subset counts after haplo-HSCT. We considered 144 leukaemic patients transplanted in the period 2001–2012. Pre-transplantation clinical variables and differential immune-cell counts (CD3, CD4, CD8 T cells, NK and B cells) measured before day 100 were evaluated for their capacity to predict overall survival, relapse mortality or non-relapse mortality (NRM). Negative prognostic factors for overall survival were advanced disease state at transplantation, host age and CMV seropositivity. Higher CD3, CD4 and CD8 counts were associated with a better overall survival and a lower NRM. Strikingly, when tested in multivariable analysis, higher CD3 and CD8 counts were still significantly associated with a lower NRM. These results indicate that an accelerated T-cell reconstitution correlates with less transplantation mortality, likely due to the protective role of T cells against viral infections. This observation suggests that CD8+ T-cell counts should be investigated as surrogate biomarkers of outcome in prospective haplo-HSCT trials.
Lingua originaleInglese
pagine (da-a)867-876
Numero di pagine10
RivistaBone Marrow Transplantation
Volume54
DOI
Stato di pubblicazionePubblicato - 2019

Keywords

  • HSCT

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