Notch-1 Controls the Expression of Fatty Acid-activated Transcription Factors and Is Required for Adipogenesis

Garcés, Cármen; Ruiz-Hidalgo, Marı́a José; Mora, Jaime Font de; Park, Crystal L.; Miele, Lucio; Goldstein, Julia; Bonvini, Ezio; Porrás, Almudena; Laborda, Jorge

doi:10.1074/jbc.272.47.29729

Cited by 144 publications

(139 citation statements)

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“…Specific strategies that selectively target individual Notch receptors include antisense (Garces et al, 1997;Shelly et al, 1999;Yasutomo et al, 2000;Weijzen et al, 2002a;Weijzen et al, 2003), RNA interference (LM, unpublished) and monoclonal antibodies (Yasutomo et al, 2000), while pharmacological small-molecule inhibitors of individual Notch receptors have not been described yet. Nonselective strategies include soluble receptor decoys that act by sequestering Notch ligands (Garces et al, 1997;Nickoloff et al, 2002) and pharmacological inhibitors of gamma-secretase (Weijzen et al, 2002a), which prevent the second ligand-induced proteolytic cleavage of Notch receptors. These agents simultaneously target all Notch receptors (Mizutani et al, 2001).…”

Section: Pharmacological and Genetic Strategies To Manipulate Notch Smentioning

confidence: 99%

“…Phosphorylation of intracellular Notch by GSK-3b (Foltz et al, 2002) and possibly by other, unspecified kinases (Ronchini and Capobianco, 2000;Shimizu et al, 2000;Ingles-Esteve et al, 2001) has been described and may contribute to regulating the half-life of Notch intracellular proteins. Notch target genes include among others helix-loop-helix inhibitory transcription factors of the hairy enhancer of split (HES) family (Enhancer of Split in Drosophila) (ArtavanisTsakonas et al, 1999) that modulate differentiation, cell cycle mediators such as p21 cip1/waf1 (Rangarajan et al, 2001b) and cyclin D1 (Ronchini and Capobianco, 2001), as well as NF-kB family (Cheng et al, 2001) and PPAR family (Garces et al, 1997;Nickoloff et al, 2002) transcription factors. Putative nontranscriptional effects of Notch signaling include direct activation of NF-kB by Notch ligands and inhibition of JNK activation Zecchini et al, 1999).…”

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confidence: 99%

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Notch signaling as a therapeutic target in cancer: a new approach to the development of cell fate modifying agents

2003

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Section: Pharmacological and Genetic Strategies To Manipulate Notch Smentioning

confidence: 99%

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Notch signaling as a therapeutic target in cancer: a new approach to the development of cell fate modifying agents

2003

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“…2D, lanes 2 and 3). To determine the specificity of this interaction, Notch-Jagged contact between CD34 + and BMEC cells was inhibited by blocking Notch receptors with an antibody directed to the extracellular domain of Notch1 (N1ab) [27,28], or with the soluble form of Notch ligand Delta4 (Dll4-Fc) [22]. Both reagents can bind to N1 and N2; antibodies directed to ligand binding region of Notch receptors and soluble ligand-fusion proteins have been used as antagonist to inhibit the full physiologic ligand-receptor binding and activation [dontu27, [37][38][39][40].…”

Section: Upregulation Of J2 On Bm Endothelial Cells Promotes Expansiomentioning

confidence: 99%

“…a) CD34 + and BMEC cocultures were grown for 5 days in the presence or absence of 2uM γ-secretase inhibitor GSI (GSI X, Calbiochem). b) Prior to seeding, CD34 + cells were blocked for 10 min on ice with human immunoglobulins (Sigma) and then incubated with saturating concentrations (25ug/ml) of soluble Dll4-Fc generated as described [22], the monoclonal antibody anti-N1 (Biomeda) [27,28] or Fc fragment control (Sigma) for 1 hour on ice. The CD34 + fraction adherent to BMEC was harvested (using 1 rinse of PBS and 1 rinse of PBS/EDTA) and used for further analysis after 24 hours (for western blot analysis) or 3 days (for colony assay).…”

Section: Cells and Cell Culturesmentioning

confidence: 99%

Tumor necrosis factor-α and endothelial cells modulate Notch signaling in the bone marrow microenvironment during inflammation

Fernández

Rodríguez

Huang

et al. 2008

Experimental Hematology

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Objective-Homeostasis of the hematopoietic compartment is challenged and maintained during conditions of stress by mechanisms that are poorly defined. To understand how the bone marrow (BM) microenvironment influences hematopoiesis, we explored the role of Notch signaling and bone marrow endothelial cells in providing microenvironmental cues to hematopoietic cells in the presence of inflammatory stimuli.Methods-The human BM endothelial cell line BMEC and primary human BM endothelial cells were analyzed for expression of Notch ligands and the ability to expand hematopoietic progenitors in an in vitro co-culture system. In vivo experiments were carried out to identify modulation of Notch signaling in BM endothelial and hematopoietic cells in mice challenged with TNFα or LPS, or in Tie2-tmTNFα transgenic mice characterized by constitutive TNFα activation.Results-BM endothelial cells were found to express Jagged ligands and to greatly support progenitor's colony-forming ability. This effect was markedly decreased by Notch antagonists and augmented by increasing levels of Jagged2. Physiologic upregulation of Jagged2 expression on BMEC was observed upon TNFα activation. Injection of TNFα or LPS upregulated 3 to 4 fold Jagged2 expression on murine BM endothelial cells in vivo and resulted in increased Notch

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“…One of the best-characterized examples involving lateral protein-protein interaction of transmembrane proteins is provided by the Notch-Delta or Notch-Serrate/Jagged systems that play pivotal roles in cell fate determination during neurogenesis (24). Recently, Notch-1 was also shown to be implicated in adipocyte differentiation (25). The organization of the pref-1 gene and the structure of the individual EGF-like repeats strongly suggest that Pref-1 is most closely related to the Delta family (26).…”

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confidence: 99%

Insulin-like Growth Factor-1/Insulin Bypasses Pref-1/FA1-mediated Inhibition of Adipocyte Differentiation

Zhang

Nøhr

Jensen

et al. 2003

Journal of Biological Chemistry

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Pref-1 is a highly glycosylated Delta-like transmembrane protein containing six epidermal growth factorlike repeats in the extracellular domain. Pref-1 is abundantly expressed in preadipocytes, but expression is down-regulated during adipocyte differentiation. Forced expression of Pref-1 in 3T3-L1 cells was reported to inhibit adipocyte differentiation. Here we show that efficient and regulated processing of Pref-1 occurs in 3T3-L1 preadipocytes releasing most of the extracellular domain as a 50-kDa heterogeneous protein, previously isolated and characterized as FA1. Unexpectedly, we found that forced expression of the soluble form, FA1, or full-length Pref-1 did not inhibit adipocyte differentiation of 3T3-L1 cells when differentiation was induced by standard treatment with methylisobutylxanthine, dexamethasone, and high concentrations of insulin. However, forced expression of either form of Pref-1/FA1 in 3T3-L1 or 3T3-F442A cells inhibited adipocyte differentiation when insulin or insulin-like growth factor-1 (IGF-1) was omitted from the differentiation mixture. We demonstrate that the level of the mature form of the IGF-1 receptor is reduced and that IGF-1-dependent activation of p42/p44 mitogen-activated protein kinases (MAPKs) is compromised in preadipocytes with forced expression of Pref-1. This is accompanied by suppression of clonal expansion and terminal differentiation. Accordingly, supplementation with insulin or IGF-1 rescued p42/p44 MAPK activation, clonal expansion, and adipocyte differentiation in a dose-dependent manner.

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Notch-1 Controls the Expression of Fatty Acid-activated Transcription Factors and Is Required for Adipogenesis

Cited by 144 publications

References 57 publications

Notch signaling as a therapeutic target in cancer: a new approach to the development of cell fate modifying agents

Notch signaling as a therapeutic target in cancer: a new approach to the development of cell fate modifying agents

Tumor necrosis factor-α and endothelial cells modulate Notch signaling in the bone marrow microenvironment during inflammation

Insulin-like Growth Factor-1/Insulin Bypasses Pref-1/FA1-mediated Inhibition of Adipocyte Differentiation

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