Effect of antiangiogenic therapy on tumor growth, vasculature and kinase activity in basal- and luminal-like breast cancer xenografts
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https://hdl.handle.net/10037/25671Date
2012-03-31Type
Journal articleTidsskriftartikkel
Peer reviewed
Author
Lindholm, Evita Maria; Kristian, Alexandr; Nalwoga, Hawa; Kruger, Kristi; Nygård, Ståle; Akslen, Lars A.; Mælandsmo, GunhildAbstract
Several clinical trials have investigated the efficacy of bevacizumab in breast cancer, and
even if growth inhibiting effects have been registered when antiangiogenic treatment is
given in combination with chemotherapy no gain in overall survival has been observed.
One reason for the lack of overall survival benefit might be that appropriate criteria for selection of patients likely to respond to antiangiogenic therapy in combination with chemotherapy, are not available.
To determine factors of importance for antiangiogenic treatment response and/or resistance, two representative human basal- and luminal-like breast cancer xenografts were
treated with bevacizumab and doxorubicin alone or in combination. In vivo growth inhibition, microvessel density (MVD) and proliferating tumor vessels (pMVD ¼ proliferative microvessel density) were analysed, while kinase activity was determined using the PamChip
Tyrosine kinase microarray system.
Results showed that both doxorubicin and bevacizumab inhibited basal-like tumor growth
significantly, but with a superior effect when given in combination. In contrast, doxorubicin inhibited luminal-like tumor growth most effectively, and with no additional benefit of
adding antiangiogenic therapy. In agreement with the growth inhibition data, vascular
characterization verified a more pronounced effect of the antiangiogenic treatment in
the basal-like compared to the luminal-like tumors, demonstrating total inhibition of
pMVD and a significant reduction in MVD at early time points (three days after treatment)
and sustained inhibitory effects until the end of the experiment (day 18). In contrast,
luminal-like tumors only showed significant effect on the vasculature at day 10 in the tumors having received both doxorubicin and bevacizumab.
Kinase activity profiling in both tumor models demonstrated that the most effective
treatment in vivo was accompanied with increased phosphorylation of kinase substrates of growth control and angiogenesis, like EGFR, VEGFR2 and PLCg1. This may be a result
of regulatory feedback mechanisms contributing to treatment resistance, and may
suggest response markers of value for the prediction of antiangiogenic treatment
efficacy.
Citation
Lindholm EM, Kristian A, Nalwoga H, Kruger K, Nygård S, Akslen LA, Mælandsmo GM, Engebråten O. Effect of antiangiogenic therapy on tumor growth, vasculature and kinase activity in basal- and luminal-like breast cancer xenografts. Molecular Oncology. 2012;6(4):418-427Metadata
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Copyright 2012 Federation of European Biochemical Societies.