Platelet-derived growth factor and basic fibroblast growth factor regulate cell proliferation and the expression of notch-1 receptor in a new oligodendrocyte cell line

Bongarzone, Ernesto R.; Byravan, Sujatha; Givogri, Maria I.; Schonmann, Vilma; Campagnoni, Anthony T.

doi:10.1002/1097-4547(20001101)62:3<319::aid-jnr1>3.0.co;2-g

Cited by 28 publications

(21 citation statements)

References 36 publications

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“…It was reported that PDGF signaling regulates the expression of Notch-1 receptor in other cell lines (20). Notch-1 signaling is known to play important roles in maintaining the balance between cell proliferation, differentiation, and apoptosis (26).…”

Section: Down-regulation Of Pdgf-d Inhibits Angiogenesismentioning

confidence: 99%

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Down-regulation of Platelet-Derived Growth Factor-D Inhibits Cell Growth and Angiogenesis through Inactivation of Notch-1 and Nuclear Factor-κB Signaling

et al. 2007

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Section: Down-regulation Of Pdgf-d Inhibits Angiogenesismentioning

confidence: 99%

“…It has been reported that Notch-1 is critically involved in the processes of tumor cell proliferation and apoptosis (19). PDGF-A has been shown to activate the expression of Notch-1 in certain cell lines (20). Therefore, we investigated whether Notch-1 was down-regulated by PDGF-D siRNA in pancreatic cancer cell lines.…”

Section: Cancer Researchmentioning

confidence: 99%

Down-regulation of Platelet-Derived Growth Factor-D Inhibits Cell Growth and Angiogenesis through Inactivation of Notch-1 and Nuclear Factor-κB Signaling

et al. 2007

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“…This reduction did not require FGF2 treatment and was not altered by expression of FGFRdn to disrupt FGFR signaling. Therefore, although FGF2 has been shown to increase Notch1 expression [4,5], Notch1 expression may already be sufficient so that FGF2 treatment does not regulate Jagged1 inhibition of OP differentiation in this context. Conversely, FGF2 treatment markedly reduced O1 acquisition among GFP+ cells in OP cell cultures or among OP cells co-cultured with Jagged1-expressing fibroblasts (Figure 1 D, b and c; 1 E).…”

Section: Resultsmentioning

confidence: 95%

“…FGF2 can induce Notch1 expression in neuroepithelial precursor cells and in a cell line with an immature oligodendrocyte phenotype [4,5]. Conversely, Notch1 signaling can increase responsiveness to FGF2 in telecephalic progenitors [24].…”

Section: Introductionmentioning

confidence: 99%

Interaction of fibroblast growth factor 2 (FGF2) and notch signaling components in inhibition of oligodendrocyte progenitor (OP) differentiation

Zhou

Armstrong

2007

Neuroscience Letters

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Oligodendrocyte progenitor (OP) cell differentiation is a critical process of developmental myelination, tumor formation, and remyelination in the CNS. Activation of the fibroblast growth factor 2 (FGF2) or notch pathway can inhibit differentiation of OP cells. The current study examines the interaction of FGF2 and notch signaling components in regulating OP differentiation. Cultured neonatal rat brain OP cells were used for transfection-based promoter assays and for infection with retroviruses expressing a GFP reporter to monitor OP differentiation into oligodendrocytes or astrocytes. FGF2 treatment resulted in a 4-fold increase of transcriptional activity from the promoter region of Hes5, a notch pathway target gene. FGF2 inhibition of OP differentiation into oligodendrocytes was perturbed by retroviral expression of a dominant negative construct for mastermind-like 1, which is an important co-activator of transcription for notch target genes. OP differentiation into oligodendrocytes was reduced by co-culture with fibroblasts expressing Jagged1, a ligand for notch receptors. This Jagged1 inhibition of OP differentiation was not altered by retroviral expression of a dominant negative FGF receptor construct. Constitutive activation of notch signaling, by retroviral expression of the Notch1 intracellular domain, greatly reduced OP differentiation into either oligodendrocytes or astrocytes and did not require FGF2 signaling. These findings indicate that inhibition of OP differentiation through the Notch1 pathway was not influenced by FGF2 signaling. However, FGF2 signaling may interact with down stream components of the notch signaling pathway, including mastermind-like1 and Hes5, to inhibit OP differentiation into oligodendrocytes.

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“…The surviving mice develop a number of defects including oligodendrocyte deficiency, lack of alveolar smooth muscle cells, lack of testicular leydig cells and a disturbance of intestinal villus formation (Betsholtz et al 2001). In an oligodendroglial cell line the treatment of cells with PDGFAA resulted in the increased expression and polarization of the notch-1 receptor (Bongarzone et al 2000), which is important in maintaining cells in an undifferentiated state (Lardelli et al 1995, Simpson 1998. Therefore, it is likely that cross-talk between PDGFAA and the notch signaling pathways maintain the pancreatic progenitor cells in an undifferentiated state, allowing regeneration in the adult.…”

Section: Discussionmentioning

confidence: 99%

Growth factor-induced signaling of the pancreatic epithelium

Kayali

Stotland

Gunst

et al. 2005

Journal of Endocrinology

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Activated signaling proteins regulate diverse processes, including the differentiation of the pancreatic islet cells during ontogeny. Here we uncover the in vivo phosphorylation status of major growth factor-activated signaling proteins in normal adult mice and during pancreatic islet regeneration. We report elevated phospho-mitogenactivated protein kinase (phospho-MAPK), phospho-cJun-NH 2 -terminal kinase (phospho-JNK), and phosphop38 MAPK expression during pancreatic regeneration. Immunoblotting experiments demonstrated elevated phosphorylation of p52 Src-homology/collagen (SHC) in the ductal network as well, substantiating the activation of this pathway. Furthermore, protein kinase B (PKB/Akt), a key signaling protein in the anti-apoptotic pathway, was phosphorylated to a greater extent in the ductal network from regenerating pancreas. We observed fibroblast growht factor (FGF)10 and platelet-derived growth factor (PDGF)AA expression in embryonic as well as regenerating adult pancreas. Epidermal growth factor (EGF) and PDGFAA stimulated MAPK and Akt phosphorylation, while FGF10 stimulated MAPK but not Akt phosphorylation in a time-dependent manner in freshly isolated cells from the adult ductal network. These data suggest that a heightened level of expression and stimulation of key signaling proteins underlie the expansion and differentiation processes that support pancreatic ontogeny and regeneration.

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Platelet-derived growth factor and basic fibroblast growth factor regulate cell proliferation and the expression of notch-1 receptor in a new oligodendrocyte cell line

Cited by 28 publications

References 36 publications

Down-regulation of Platelet-Derived Growth Factor-D Inhibits Cell Growth and Angiogenesis through Inactivation of Notch-1 and Nuclear Factor-κB Signaling

Down-regulation of Platelet-Derived Growth Factor-D Inhibits Cell Growth and Angiogenesis through Inactivation of Notch-1 and Nuclear Factor-κB Signaling

Interaction of fibroblast growth factor 2 (FGF2) and notch signaling components in inhibition of oligodendrocyte progenitor (OP) differentiation

Growth factor-induced signaling of the pancreatic epithelium

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