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10 research outputs found

Insulin growth factor 1 like receptor (IGF-1R)

Author: A Chakravarti
A Girnita
A Sawano
B Ozanne
CH Chung
CR Leemans
DL Wheeler
DL Wheeler
DR Clayburgh
Eric Armstrong
F Pietrantonio
Gopal Iyer
GW Allen
J Baker
J Li
J Tabernero
J-H Klusmann
JA Bonner
JA Krall
James Price
JH Hanke
JP Dawson
JS Biscardi
JS Logue
K Azuma
KI Sato
KL Mueller
L Arteaga Carlos
LH Defize
LP Stabile
M Pollak
M Shoyab
MJ Jameson
MS Kies
NE Bhola
OT Dale
P Koppikar
Paul M. Harari
PM Harari
R Nahta
R-H Tao
S Benavente
S K-i
S Pan
S-C Yin
Shay Bourgeois
Shyhmin Huang
The Cancer Genome Atlas N
Publication venue: 'Springer Science and Business Media LLC'
Publication date
Field of study

Enhancement of radiation response with bevacizumab

Author: Armstrong Eric
Eickhoff Jens C
Harari Paul M
Hoang Tien
Huang Shyhmin
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/04/2012
Field of study

Abstract Background Vascular endothelial growth factor (VEGF) plays a critical role in tumor angiogenesis. Bevacizumab is a humanized monoclonal antibody that neutralizes VEGF. We examined the impact on radiation response by blocking VEGF signaling with bevacizumab. Methods Human umbilical vein endothelial cell (HUVEC) growth inhibition and apoptosis were examined by crystal violet assay and flow cytometry, respectively. In vitro HUVEC tube formation and in vivo Matrigel assays were performed to assess the anti-angiogenic effect. Finally, a series of experiments of growth inhibition on head and neck (H&N) SCC1 and lung H226 tumor xenograft models were conducted to evaluate the impact of bevacizumab on radiation response in concurrent as well as sequential therapy. Results The anti-angiogenic effect of bevacizumab appeared to derive not only from inhibition of endothelial cell growth (40%) but also by interfering with endothelial cell function including mobility, cell-to-cell interaction and the ability to form capillaries as reflected by tube formation. In cell culture, bevacizumab induced a 2 ~ 3 fold increase in endothelial cell apoptosis following radiation. In both SCC1 and H226 xenograft models, the concurrent administration of bevacizumab and radiation reduced tumor blood vessel formation and inhibited tumor growth compared to either modality alone. We observed a siginificant tumor reduction in mice receiving the combination of bevacizumab and radiation in comparison to mice treated with bevacizumab or radiation alone. We investigated the impact of bevacizumab and radiation treatment sequence on tumor response. In the SCC1 model, tumor response was strongest with radiation followed by bevacizumab with less sequence impact observed in the H226 model. Conclusions Overall, these data demonstrate enhanced tumor response when bevacizumab is combined with radiation, supporting the emerging clinical investigations that are combining anti-angiogenic therapies with radiation.</p

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