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High CD34 surface expression in BCP-ALL predicts poor induction therapy response and is associated with altered expression of genes related to cell migration and adhesion

  • Signe Modvig*
  • , Rasmus Wernersson
  • , Nina Friesgaard Øbro
  • , Lars Rønn Olsen
  • , Claus Christensen
  • , Susanne Rosthøj
  • , Matilda Degn
  • , Gitte Wullf Jürgensen
  • , Hans O. Madsen
  • , Birgitte Klug Albertsen
  • , Peder Skov Wehner
  • , Steen Rosthøj
  • , Henrik Lilljebjörn
  • , Thoas Fioretos
  • , Kjeld Schmiegelow
  • , Hanne Vibeke Marquart
  • *Kontaktforfatter

Publikation: Bidrag til tidsskriftTidsskriftartikelForskningpeer review

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Abstract

Minimal residual disease (MRD) constitutes the most important prognostic factor in B-cell precursor acute lymphoblastic leukemia (BCP-ALL). Flow cytometry is widely used in MRD assessment, yet little is known regarding the effect of different immunophenotypic subsets on outcome. In this study of 200 BCP-ALL patients, we found that a CD34-positive, CD38 dim-positive, nTdT dim-positive immunophenotype on the leukemic blasts was associated with poor induction therapy response and predicted an MRD level at the end of induction therapy (EOI) of ≥ 0.001. CD34 expression was strongly and positively associated with EOI MRD, whereas CD34-negative patients had a low relapse risk. Further, CD34 expression increased from diagnosis to relapse. CD34 is a stemness-associated cell-surface molecule, possibly involved in cell adhesion/migration or survival. Accordingly, genes associated with stemness were overrepresented among the most upregulated genes in CD34-positive leukemias, and protein–protein interaction networks showed an overrepresentation of genes associated with cell migration, cell adhesion, and negative regulation of apoptosis. The present work is the first to demonstrate a CD34-negative immunophenotype as a good prognostic factor in ALL, whereas high CD34 expression is associated with poor therapy response and an altered gene expression profile reminiscent of migrating cancer stem-like cells.

OriginalsprogEngelsk
TidsskriftMolecular Oncology
Vol/bind16
Udgave nummer10
Sider (fra-til)2015-2030
Antal sider16
ISSN1574-7891
DOI
StatusUdgivet - maj 2022

Bibliografisk note

© 2022 The Authors. Molecular Oncology published by John Wiley & Sons Ltd on behalf of Federation of European Biochemical Societies.

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