2002
DOI: 10.1074/jbc.m204527200
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Regulation of Wnt Signaling during Adipogenesis

Abstract: We have identified Wnt10b as a potent inhibitor of adipogenesis that must be suppressed for preadipocytes to differentiate in vitro. Here, we demonstrate that a specific inhibitor of glycogen synthase kinase 3, CHIR 99021, mimics Wnt signaling in preadipocytes. CHIR 99021 stabilizes free cytosolic ␤-catenin and inhibits adipogenesis by blocking induction of CCAAT/enhancer-binding protein ␣ and peroxisome proliferatoractivated receptor ␥. Preadipocyte differentiation is inhibited when 3T3-L1 cells are exposed t… Show more

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Cited by 673 publications
(657 citation statements)
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“…Overexpression of Hoxd4 in the cartilage of transgenic mice has been found to reduce expression of Wnt3a, a canonical Wnt pathway ligand, suggesting a functional role for this homeobox transcription factor in multipotential stem cells capable of undergoing adipogenesis or chondrogenesis and a potential relationship to Wnt-related mechanisms (Kruger and Kappen 2010). This interpretation would be consistent with earlier studies determining that Wnt10b, another canonical Wnt pathway ligand, suppressed adipogenesis and promoted osteogenesis in multipotential stem cell models (Ross et al 2000;Bennett et al 2002Bennett et al , 2005.…”
Section: Discussionsupporting
confidence: 86%
“…Overexpression of Hoxd4 in the cartilage of transgenic mice has been found to reduce expression of Wnt3a, a canonical Wnt pathway ligand, suggesting a functional role for this homeobox transcription factor in multipotential stem cells capable of undergoing adipogenesis or chondrogenesis and a potential relationship to Wnt-related mechanisms (Kruger and Kappen 2010). This interpretation would be consistent with earlier studies determining that Wnt10b, another canonical Wnt pathway ligand, suppressed adipogenesis and promoted osteogenesis in multipotential stem cell models (Ross et al 2000;Bennett et al 2002Bennett et al , 2005.…”
Section: Discussionsupporting
confidence: 86%
“…Other evidence for a role of the Wnt/ β-catenin pathway in regulating mesenchymal stem cell differentiation is illustrated by the genetic deletion of the Wnt antagonist Sfrp1, which leads to a 20% reduction in body fat concomitant with increased bone mass [41]. Furthermore, treatments with pharmacological inhibitors of GSK-3β stabilize intracellular β-catenin, thereby stimulating osteoblastogenesis and blocking adipocyte differentiation [42,43]. In the present study, disruption of the interaction of Axin and β-catenin by a small molecule, rather than inhibition of GSK-3β activity, promoted mesenchymal precursors to differentiate into osteoblasts and restrained adipocyte differentiation, mimicking the activation of the Wnt/β-catenin pathway.…”
Section: Discussionmentioning
confidence: 99%
“…This factor has been shown to repress adipogenesis by blocking PPARG and CEPBA induction by stabilizing β-catenin, which interacts transcriptionally to activate Wnt target gene expression (Bennet et al, 2002), although the molecular mechanism by which Wnt/β-catenin signalling suppresses the expression of these two genes is poorly understood. The overexpression of WNT10B observed in the LM seems to agree with the low level of development of the IM AT as represented by the small amount of IM chemical fat and small adipocyte size.…”
Section: Marbling and Adipositymentioning
confidence: 99%