par Ceelen, Wim;Boterberg, Tom;Smeets, Peter;Van Damme, Nicole 
;Demetter, Pieter ;Zwaenepoel, O;Cesteleyn, L;Houtmeyers, Philippe;Peeters, Marc;Pattyn, Piet
Référence British Journal of Cancer, 96, 5, page (692-700)
Publication Publié, 2007-03
;Demetter, Pieter ;Zwaenepoel, O;Cesteleyn, L;Houtmeyers, Philippe;Peeters, Marc;Pattyn, PietRéférence British Journal of Cancer, 96, 5, page (692-700)
Publication Publié, 2007-03
Article révisé par les pairs
| Résumé : | Recent data suggest that recombinant human erythropoietin (rhEPO) modulates tumour growth and therapy response. The purpose of the present study was to examine the modulation of radiotherapy (RT) effects on tumour microvessels by rhEPO in a rat colorectal cancer model. Before and after 5 x 5 Gy of RT, dynamic contrast-enhanced -magnetic resonance imaging was performed and endothelial permeability surface product (PS), plasma flow (F), and blood volume (V) were modelled. Imaging was combined with pO(2) measurements, analysis of microvessel density, microvessel diameter, microvessel fractal dimension, and expression of vascular endothelial growth factor (VEGF), hypoxia-inducible factor-1 alpha (HIF-1alpha), Bax, and Bcl-2. We found that RT significantly reduced PS and V in control rats, but not in rhEPO-treated rats, whereas F was unaffected by RT. Oxygenation was significantly better in rhEPO-treated animals, and RT induced a heterogeneous reoxygenation in both groups. Microvessel diameter was significantly larger in rhEPO animals, whereas VEGF expression was significantly lower in the rhEPO group. No differences were observed in HIF-1alpha, Bax, or Bcl-2 expression. We conclude that rhEPO results in spatially heterogeneous modulation of RT effects on tumour microvessels. Direct effects of rhEPO on neoplastic endothelium are likely to explain these findings in addition to indirect effects induced by increased oxygenation. |
