Folia Histochemica et Cytobiologica (Mar 2007)

CD40L and IL-4 stimulation of acute lymphoblastic leukemia cells results in upregulation of mRNA level of FLICE--an important component of apoptosis.

  • Radosław Jaworowski,
  • Igor Olejnik,
  • Tomasz Szczepalński,
  • Andrzej Kołtan,
  • Iwona Malinowska,
  • Maryna Krawczuk-Rybak,
  • Anna Stasiak-Barmuta,
  • Elibieta Iłendo,
  • Oksana Kowalczuk,
  • Włodzimierz łuczyński,
  • Lech Chyczewski,
  • Michał Matysiak,
  • Mariusz Wysocki,
  • Danuta Sońta-Jakimczyk,
  • Maria Wieczorek

DOI
https://doi.org/10.5603/4545
Journal volume & issue
Vol. 45, no. 1
pp. 15 – 20

Abstract

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The use of cancer vaccines based on dendritic cells (DC) presenting tumor antigens can be a promising tool in the treatment of leukemia. The functional characteristics of leukemia derived DC is still to be elucidated. CD40 promotes survival, proliferation and differentiation of normal B cells. CD40 triggering was used to enhance the poor antigen-presenting capacity of leukemic B-cells. Since it is still unclear whether CD40 ligation drives neoplastic B-cells to apoptosis or not, we assessed the mRNA expression of FLICE, FAS, FADD and TRADD - important components of apoptosis machinery, using real-time PCR in acute lymphoblastic leukemia cells before and after CD40 and IL-4 stimulation. ALL cells stimulated with CD40L/IL-4 expressed dendritic cell phenotype at mRNA and protein levels (upregulation of main costimulatory and adhesion molecules noted in real-time RT PCR and flow cytometry); they also expressed higher amounts of mRNA for FLICE, TRADD and FADD after CD40L/IL-4 stimulation. However differences statistically significant comparing cells cultured with CD40L/IL-4 and medium alone regarded only FLICE. Concluding, we showed upregulation of important elements of apoptosis at mRNA level in ALL cells after CD40 ligation.