Comparison of the intracellular signaling responses by three chimeric fibroblast growth factor receptors in PC12 cells

Raffioni, Simona; Thomas, Dominique; Foehr, Erik D; Thompson, Leslie M.; Bradshaw, Ralph A.

doi:10.1073/pnas.96.13.7178

Cited by 69 publications

(65 citation statements)

References 31 publications

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“…FGFR1 and FGFR3 have different signaling properties in some cell types in vitro (Wang et al 1994;Lin et al 1996;Naski et al 1996). These differences may be attributable to differences in the strength of the tyrosine kinase signal but not to the specific signaling pathway activated (Raffioni et al 1999). Consistent with this, both receptor kinase domains appear to have similar activities when expressed in proliferating chondrocytes in vivo (Wang et al 2001).…”

Section: Response Of the Chondrocyte To Fgf Signalingsupporting

confidence: 54%

FGF signaling pathways in endochondral and intramembranous bone development and human genetic disease

Ornitz¹,

Marie²

2002

Genes Dev.

808

648

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Over the last decade the identification of mutations in the receptors for fibroblast growth factors (FGFs) has defined essential roles for FGF signaling in both endochondral and intramembranous bone development. FGF signaling pathways are essential for the earliest stages of limb development and throughout skeletal development. In this review, we examine the role of FGF signaling in bone development and in human genetic diseases that affect bone development. We also explore what is presently known about how FGF signaling pathways interact with other major signaling pathways that regulate chondrogenesis and osteogenesis.

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Section: Response Of the Chondrocyte To Fgf Signalingsupporting

confidence: 54%

FGF signaling pathways in endochondral and intramembranous bone development and human genetic disease

Ornitz¹,

Marie²

2002

Genes Dev.

808

648

View full text Add to dashboard Cite

show abstract

“…Both FGFR1 and FGFR3 kinase domains appear to have similar activities when expressed in growth plate chondrocytes in vivo [115]. Therefore, observed differences between these receptors must be attributable to differences in the strength of the tyrosine kinase signal rather than the specific signaling pathway activated [116]. This property of FGF signaling in chondrocytes supports the hypothesis that the proliferating chondrocyte itself is uniquely responsive to an FGFR signal.…”

supporting

confidence: 58%

FGF signaling in the developing endochondral skeleton

Ornitz¹

2005

Cytokine & Growth Factor Reviews

320

259

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Mutations in fibroblast growth factor receptors (Fgfrs) are the etiology of many craniosynostosis and chondrodysplasia syndromes in humans. The phenotypes associated with these human syndromes and the phenotypes resulting from targeted mutagenesis in the mouse have defined essential roles for FGF signaling in both endochondral and intramembranous bone development. In this review, I will focus on the role of FGF signaling in chondrocytes and osteoblasts and how FGFs regulate the growth and development of endochondral bone. KeywordsFGF; Skeletal development; Craniosynostosis; Achondroplasia; Receptor tyrosine kinase Human skeletal disease syndromes: the FGF connectionFgfrs were known to be expressed in the developing skeleton. However, a functional link between FGF signaling and skeletal development was not appreciated until the discovery that achondroplasia (ACH), the most common form of skeletal dwarfism in humans, was caused by a missense mutation in Fgfr3 [1][2][3][4][5]. Following this initial discovery, a milder form of dwarfism, hypochondroplasia (HCH) [6,7], and a more severe form of dwarfism, thanatophoric dysplasia (TD) [3,[8][9][10], were also found to result from mutations in Fgfr3.In addition to the chondrodysplasia syndromes, many other human skeletal dysplasias have been attributed to mutations in Fgfrs 1, 2 and 3 [11][12][13][14][15][16][17]. These disorders have in common craniosynostosis (premature fusion of the cranial sutures) and variably other phenotypes that affect the appendicular skeleton and other organ systems. The craniosynostosis syndromes involving Fgfr2 include Apert syndrome (AS) [18], Beare-Stevenson cutis gyrata [19], Crouzon syndrome (CS) [20][21][22][23][24][25][26][27][28][29][30][31][32], Pfeiffer syndrome (PS) [33][34][35][36][37]23,28,29], Jackson-Weiss syndrome (JWS) [22,23,26] and a non-syndromic craniosynostosis (NSC) [38]. Recently a family has been described with a double mutation in Fgfr2 (S2521, A315S) that is associated with syndactyly but not craniosynostosis [39]. However, individually, these mutations are associated with low-penetrance craniosynostosis.In addition to the single mutation in Fgfr1 (P252R) that causes Pfeiffer syndrome [40][41][42]29], a rare mutation has been identified that causes osteoglophonic dysplasia (OD), a disease characterized by craniosynostosis, prominent supraorbital ridge, and depressed nasal bridge, as well as the rhizomelic dwarfism and nonossifying bone lesions [43]. One patient has also been described with Jackson-Weiss syndrome and a P252R mutation in Fgfr1 Recently, a mutation in Fgfr3 (P250R) has been described that causes Muenke syndrome (MS), which is characterized by craniosynostosis and variably other skeletal and neurological phenotypes [38,46,47]. Another mutation in Fgfr3 (A391E) causes Crouzon syndrome with acanthosis nigricans, now referred to as crouzonodermoskeletal syndrome [48][49][50][51][52]24].All of the skeletal disease syndromes are caused by autosomal dominant mutations and frequently arise sporadically...

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“…With respect to TrkA, it has been shown that Shc is required for this pathway (13,34,38). The failure of Shc to compete for with p62 for binding to TrkA reveals that p62 activates the B pathway independently of this site.…”

Section: Discussionmentioning

confidence: 99%

Association of the Atypical Protein Kinase C-interacting Protein p62/ZIP with Nerve Growth Factor Receptor TrkA Regulates Receptor Trafficking and Erk5 Signaling

Geetha

Wooten

2003

Journal of Biological Chemistry

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Comparison of the intracellular signaling responses by three chimeric fibroblast growth factor receptors in PC12 cells

Cited by 69 publications

References 31 publications

FGF signaling pathways in endochondral and intramembranous bone development and human genetic disease

FGF signaling pathways in endochondral and intramembranous bone development and human genetic disease

FGF signaling in the developing endochondral skeleton

Association of the Atypical Protein Kinase C-interacting Protein p62/ZIP with Nerve Growth Factor Receptor TrkA Regulates Receptor Trafficking and Erk5 Signaling

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