2006
DOI: 10.1016/j.cellsig.2006.03.001
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A role for extracellular and transmembrane domains of Sef in Sef-mediated inhibition of FGF signaling

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Cited by 35 publications
(39 citation statements)
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“…These results suggest that in prostate cancer cells hSef exerts an effect at the level of the FGFR or at Ras. Functionality at this level is further supported by the consistent finding of Sef interaction (colocalisation and immunoprecipitation) with the FGFR across different species and cell types and its ability to inhibit both FGFR as well as FRS phosphorylation (Tsang et al, 2002;Kovalenko et al, 2003Kovalenko et al, , 2006Xiong et al, 2003;Yang et al, 2003;Ren et al, 2007). The ability of hSef to act upstream or at Ras would imply that it should also inhibit alternate pathways activated by FGFR/Ras interaction, which include PI3 kinase (Gioeli, 2005).…”
Section: Discussionmentioning
confidence: 64%
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“…These results suggest that in prostate cancer cells hSef exerts an effect at the level of the FGFR or at Ras. Functionality at this level is further supported by the consistent finding of Sef interaction (colocalisation and immunoprecipitation) with the FGFR across different species and cell types and its ability to inhibit both FGFR as well as FRS phosphorylation (Tsang et al, 2002;Kovalenko et al, 2003Kovalenko et al, , 2006Xiong et al, 2003;Yang et al, 2003;Ren et al, 2007). The ability of hSef to act upstream or at Ras would imply that it should also inhibit alternate pathways activated by FGFR/Ras interaction, which include PI3 kinase (Gioeli, 2005).…”
Section: Discussionmentioning
confidence: 64%
“…In contrast, the short isoform of hSef inhibited MAPK activation in both cell types. Work with the full-length mouse homologue, however, showed that Sef was capable of blocking FGF-induced cell proliferation in fibroblast cells and that this was associated with decreased phosphorylation of Raf, MEK and ERK (Kovalenko et al, 2006). In this study we were only able to focus on the function of full-length Sef and therefore cannot currently comment on the role of the short isoform in prostate cancer cells.…”
Section: Discussionmentioning
confidence: 70%
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“…In vitro, Sef overexpression induces apoptosis, whereas knockdown of Sef promotes cell migration in response to FGF ligand, but in vivo roles for Sef have not yet been described (Darby et al, 2006;Kovalenko et al, 2006). FGF2 independently affects both the proliferation and migration of cochlear nucleus precursors in vitro (Zhou et al, 1996;Hossain et al, 2006), whereas FGF8 contributes to tissue morphogenesis, proliferation, and survival in the hindbrain but is surprisingly dispensible for specific cell fate decisions here (Foucher et al, 2006).…”
Section: Discussionmentioning
confidence: 99%
“…2B). In addition, SEF, Sprouty2, PEA3 and ERM, all members of the FGF synexpression group (Brent and Tabin, 2004;Kovalenko et al, 2006), were downregulated by BMP4 treatment in AHF explants ( Fig. 2B; see Fig.…”
Section: Bmp4 Induces the Expression Of Its Synexpression Group And Smentioning
confidence: 99%