Article ID | Journal | Published Year | Pages | File Type |
---|---|---|---|---|
1983561 | The International Journal of Biochemistry & Cell Biology | 2013 | 11 Pages |
Abstract
FGFs, in a complex with their receptors (FGFRs) and heparan sulfate (HS), are responsible for a range of cellular functions, from embryogenesis to metabolism. Both germ line and somatic FGFR mutations are known to play a role in a range of diseases, most notably craniosynestosis dysplasias, dwarfism and cancer. Because of the ability of FGFR signalling to induce cell proliferation, migration and survival, FGFRs are readily co-opted by cancer cells. Mutations in, and amplifications of, these receptors are found in a range of cancers with some of the most striking clinical findings relating to their contribution to pathogenesis and progression of female cancers. Here, we outline the molecular mechanisms of FGFR signalling and discuss the role of this pathway in women's cancers, focusing on breast, endometrial, ovarian and cervical carcinomas, and their associated preclinical and clinical data. We also address the rationale for therapeutic intervention and the need for FGFR-targeted therapy to selectively target cancer cells in view of the fundamental roles of FGF signalling in normal physiology.
Keywords
FGFRTICFGFDCISAuNPTMAMSICCCCLCIDCmAbEECTKIVEGFRPDGFRRTKNEECCervical intraepithelial neoplasiaMonoclonal antibodyImmunohistochemistryIHCMicrosatellite instabilityRTK, Receptor tyrosine kinaseCinTherapyCancerClear cell carcinomaSignallingFibroblast growth factor (FGF)fibroblast growth factorFluorescence in situ hybridisationFishgenome wide association studyGWASTyrosine kinase inhibitorTissue microarrayGold nanoparticleHeparan sulfateHuman papilloma virusHPVSNPEndometrioid endometrial carcinomaDuctal carcinoma in situInvasive ductal carcinomaCISHoestrogen receptorplatelet-derived growth factor receptorvascular endothelial growth factor receptorfibroblast growth factor receptorFibroblast growth factor receptor (FGFR)Progesterone receptor
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Authors
Abbie E. Fearon, Charlotte R. Gould, Richard P. Grose,