Publication | Closed Access
Vascular endothelial growth factor-A(165) induces progression of melanoma brain metastases without induction of sprouting angiogenesis.
155
Citations
14
References
2002
Year
PathologyInduces ProgressionMalignant MelanomaAccelerated GrowthTumor BiologyVascular PermeabilityAngiogenesisMelanoma Brain MetastasesCancer Cell BiologyRadiation OncologyHealth SciencesMelanomaVascular BiologyNeovascularizationVascular Endothelial Growth FactorCell BiologyTumor MicroenvironmentMedicineCancer Growth
We investigated the mechanisms of vascularization in a brain metastases model of malignant melanoma. Parenchymal metastases expressing little vascular endothelial growth factor-A (VEGF-A) co-opted the preexistent brain vasculature, leading to an infiltrative phenotype. Metastases of the human melanoma cell line Mel57, engineered to express recombinant VEGF-A(165), showed accelerated growth in a combined expansive and infiltrative pattern with marked central necrosis. This difference in growth profile was accompanied by dilation of co-opted intra- and peritumoral vessels with concomitant induction of vascular permeability. Our data show that modulation of preexistent vasculature can contribute to malignant progression without induction of sprouting angiogenesis.
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