Fibroblast growth factors, their receptors and signaling.
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TLDR
FGF signaling also appears to play a role in tumor growth and angiogenesis, and autocrine FGF signaling may be particularly important in the progression of steroid hormone-dependent cancers to a hormone-independent state.Abstract:
Fibroblast growth factors (FGFs) are small polypeptide growth factors, all of whom share in common certain structural characteristics, and most of whom bind heparin avidly. Many FGFs contain signal peptides for secretion and are secreted into the extracellular environment, where theycan bind to the heparan-like glycosaminoglycans (HLGAGs) of the extracellular matrix (ECM). From this reservoir, FGFs mayact directlyon target cells, or theycan be released through digestion of the ECM or the activityof a carrier protein, a secreted FGF binding protein. FGFs bind specific receptor tyrosine kinases in the context of HLGAGs and this binding induces receptor dimerization and activation, ultimatelyresulting in the activation of various signal transduction cascades. Some FGFs are potent angiogenic factors and most playimportant roles in embry onic development and wound healing. FGF signaling also appears to playa role in tumor growth and angiogenesis, and autocrine FGF signaling maybe particularlyimportant in the progression of steroid hormone-dependent cancers to a hormone-independent state.read more
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References
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Journal ArticleDOI
Basic fibroblast growth factor (bFGF) dissociates rapidly from heparan sulfates but slowly from receptors. Implications for mechanisms of bFGF release from pericellular matrix.
TL;DR: The results suggest that degradative enzymes may not be needed to release bFGF from the heparan sulfates in instances where receptors and heParan sulfate-bound bF GF are in close proximity because dissociation from heparin sulfates occurs rapidly enough to allow bFGI to bind to unoccupied receptors by laws of mass action.
Journal Article
Fibroblast Growth Factor Receptor Gene Expression and Immunoreactivity Are Elevated in Human Glioblastoma Multiforme
Richard S. Morrison,Fumio Yamaguchi,Janet M. Bruner,Mark Tang,Wallace L. McKeehan,Mitchel S. Berger +5 more
TL;DR: Results indicate that glioblastoma cells, in contrast to endothelial cells within the tumor, display increased levels of FGFR1, which may be associated with increased autocrine growth activity of tumor cells and probably not related to the increased endothelial cell proliferation associated with these tumors.
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Murine cortactin is phosphorylated in response to fibroblast growth factor-1 on tyrosine residues late in the G1 phase of the BALB/c 3T3 cell cycle.
TL;DR: Immunochemical analysis of m-cortactin-tyrosine phosphorylation in response to FGF-1 demonstrates a biphasicosphorylation pattern both as a weak immediate-early and strong mid to late G1 response protein.
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Basic fibroblast growth factor is neither necessary nor sufficient for the development of retinal neovascularization.
Hiroaki Ozaki,Naoyuki Okamoto,Sagrario Ortega,Michelle Chang,Keiko Ozaki,Srinivas R. Sadda,Melissa A. Vinores,Nancy L. Derevjanik,Donald J. Zack,Claudio Basilico,Peter A. Campochiaro +10 more
TL;DR: The data indicate that FGF2 expression is not necessary nor sufficient for the development of retinal neovascularization, and suggests that agents that specifically antagonize F GF2 are not likely to be useful adjuncts in the treatment of retina neov vascularization.
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Fibroblast growth factor-5 stimulates mitogenic signaling and is overexpressed in human pancreatic cancer : evidence for autocrine and paracrine actions
TL;DR: Observations suggest that FGF-5 may participate in autocrine and paracrine pathways promoting pancreatic cancer cell growth in vivo.