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Publication : Gene expression profile in fibroblast growth factor 2-transformed endothelial cells.

First Author  Dell'Era P Year  2002
Journal  Oncogene Volume  21
Issue  15 Pages  2433-40
PubMed ID  11948428 Mgi Jnum  J:84962
Mgi Id  MGI:2670944 Doi  10.1038/sj.onc.1205301
Citation  Dell'Era P, et al. (2002) Gene expression profile in fibroblast growth factor 2-transformed endothelial cells. Oncogene 21(15):2433-40
abstractText  Fibroblast growth factor-2 (FGF2) exerts paracrine and autocrine functions on endothelial cells. FGF2-overexpressing murine aortic endothelial cells (FGF2-T-MAE cells) induce opportunistic hemangioendothelioma-like tumors when inoculated in immunodeficient mice. To evaluate the impact of FGF2-mediated activation on gene expression profile in transformed endothelial cells, we performed subtractive suppression hybridization analysis between FGF2-T-MAE cells and parental MAE cells. The two cell populations were compared for differential gene expression also by gene macroarray hybridization with 32P-labeled cDNAs. The two approaches allowed the identification of 27 transcripts whose expression was upregulated by FGF2 in endothelial cells. With the exception of one unknown gene, the differentially expressed transcripts encoded for proteins involved in the modulation of cell cycle, differentiation, and cell adhesion. Among them, the stress-inducible genes A170, GADD45 and GADD153 are upregulated by FGF2 transfection or recombinant growth factor treatment. Their expression was also induced in vascular tumors originated by parental or FGF2-transfected MAE cells in nude mice. This study extends the number of genes involved in tumor angiogenesis and/or endothelial cell transformation, a finding with possible implications for the discovery of novel targets for angiostatic therapy.
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