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Stimulation of tumour growth by wound-derived growth factors
Authors
AE Bogden
GE Peoples
+22 more
HF Dvorak
HT Deelman
IF Pollack
JC Tsai
LM Strawn
M Marikovsky
M Marikovsky
MS Murthy
MS O’Reilly
MS O’Reilly
PH Pedersen
R Abramovitch
R Abramovitch
R Abramovitch
R Abramovitch
S Frank
S Higashiyama
SE Lynch
SM Murthy
TA Libermann
V Moulin
YS Schiffenbauer
Publication date
Publisher
Nature Publishing Group
Doi
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on
PubMed
Abstract
The goal of this work was to determine the molecular basis for the induction of tumour vascularization and progression by injury. Magnetic resonance imaging (MRI) studies demonstrated that administration of wound fluid derived from cutaneous injuries in pigs reduced the lag for vascularization and initiation of growth of C6 glioma spheroids, implanted in nude mice, and accelerated tumour doubling time. The former effect can be attributed to the angiogenic capacity of wound fluid as detected in vivo by MRI, and in vitro in promoting endothelial cell proliferation. The latter effect, namely the induced rate of tumour growth, is consistent with the angiogenic activity of wound fluid as well as with the finding that wound fluid was directly mitogenic to the tumour cells, and accelerated growth of C6 glioma in spheroid culture. Of the multiple growth factors present in wound fluid, two key factors, heparin-binding epidermal growth factor (EGF)-like growth factor (HB-EGF) and platelet-derived growth factor (PDGF), were identified as the dominant mitogens for C6 glioma, and inhibition of their activity using specific neutralizing antibodies suppressed the mitogenic effect of wound fluid on DNA synthesis in C6 glioma. This study suggests that the stimulatory effect of injury on tumour progression can possibly be attenuated by therapeutic targeting directed against a limited number of specific growth factors. © 1999 Cancer Research Campaig
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Last time updated on 11/12/2019