Ligand activation of peroxisome proliferator-activated receptor β/δ (PPARβ/δ) inhibits chemically induced skin tumorigenesis

Bility, Moses T.; Devlin-Durante, Meghann; Blazanin, Nicholas; Glick, Adam B.; Ward, Jerrold M.; Kang, Boo Hyon; Kennett, Mary J.; Gonzalez, Frank J.; Peters, Jeffrey M.

doi:10.1093/carcin/bgn219

Cited by 38 publications

(83 citation statements)

References 49 publications

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“…Previous work demonstrated that activation of PPAR␤/␦ attenuated skin tumorigenesis in a 2-stage chemical carcinogenesis bioassay and inhibited proliferation of cells with a mutation in the Hras gene (3). This suggests that PPAR␤/␦ could inhibit tumorigenesis through inhibition of oncogenic Hras signaling, which was examined in these studies.…”

mentioning

confidence: 80%

“…Consistent with this phenotype, exacerbated skin tumorigenesis was also found in Ppar␤/␦-null mice following a two-stage chemical carcinogenesis bioassay (31). Subsequent studies demonstrated that ligand activation of PPAR␤/␦ inhibits chemically induced tumorigenesis (3,4,68). One mechanism that may underlie these PPAR␤/␦-dependent chemopreventive effects is modulation of epidermal cell proliferation through inhibition of protein kinase C ␣/mitogen-activated protein kinase (PKC␣/MAPK) (31,33).…”

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confidence: 83%

“…Cells were subsequently cultured in control medium or medium containing GW0742 for up to 9 days postinfection. Keratinocytes of the 308 cell line that contain an activated mutation in Hras (56, 65) were cultured as described previously (3,4).…”

Section: Methodsmentioning

confidence: 99%

“…One mechanism that may underlie these PPAR␤/␦-dependent chemopreventive effects is modulation of epidermal cell proliferation through inhibition of protein kinase C ␣/mitogen-activated protein kinase (PKC␣/MAPK) (31,33). Additionally, ligand activation of PPAR␤/␦ induces terminal differentiation (3,32,61), which influences cell proliferation and skin tumorigenesis.…”

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confidence: 99%

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Peroxisome Proliferator-Activated Receptor β/δ Cross Talks with E2F and Attenuates Mitosis in HRAS-Expressing Cells

Zhu

Khozoie

Bility

et al. 2012

Molecular and Cellular Biology

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confidence: 80%

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confidence: 83%

Section: Methodsmentioning

confidence: 99%

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confidence: 99%

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Peroxisome Proliferator-Activated Receptor β/δ Cross Talks with E2F and Attenuates Mitosis in HRAS-Expressing Cells

Zhu

Khozoie

Bility

et al. 2012

Molecular and Cellular Biology

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“…It is possible that this dual action also explains the different results concerning the influence of PPAR␦ activators in the treatment and development of various tumor entities. Recently, Bility et al demonstrated that PPAR␦ agonists inhibit chemically induced skin carcinogenesis, whereas Kim et al demonstrated that chemically induced skin carcinogenesis is not influenced by PPAR␦ (29,30). Han et al demonstrated that PPAR␦ agonists induce human lung cancer cell proliferation, whereas He et al found that they do not influence lung cancer cell proliferation (31,32).…”

Section: Discussionmentioning

confidence: 99%

Peroxisome Proliferator-activated Receptor δ Activators Induce IL-8 Expression in Nonstimulated Endothelial Cells in a Transcriptional and Posttranscriptional Manner*

Meißner

Hrgović

Doll

et al. 2010

Journal of Biological Chemistry

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It is well known that IL-8 is also regulated by mRNA stability. To provide further evidence for this concept, we performed mRNA stability assays and found that PPAR␦ agonists induce the mRNA stability of IL-8. In addition, we showed that PPAR␦ agonists induce the phosphorylation of ERK1/2 and p38, which are known to be involved in the increase of mRNA stability. The inhibition of these MAPK signaling pathways resulted in a significant suppression of the induced IL-8 expression and the reduced mRNA stability. Therefore, our data provide the first evidence that PPAR␦ induces IL-8 expression in nonstimulated endothelial cells via transcriptional as well as posttranscriptional mechanisms.Peroxisome proliferator-activated receptors (PPARs) 2 are members of the nuclear receptor/ligand-activated transcription factors superfamily and consist of three different subtypes: PPAR␣, PPAR␦, and PPAR␥. The role of these receptors was originally thought to be restricted to lipid and lipoprotein metabolism, glucose homeostasis, and cellular differentiation (1, 2). PPARs are activated by natural ligands, such as eicosanoids and fatty acids. In addition, synthetic antidiabetic thiazolidinediones and lipid-lowering fibrates have been shown to act as activators of PPAR␥ and PPAR␣, respectively (3, 4). To date, PPAR␦, which is expressed in almost all tissues, is the subtype that still remains an interesting target for new pharmaceutical drugs.New evidence suggests that PPAR␦ plays a crucial role in the regulation of differentiation, cell growth, and the metabolism of lipids and glucose (5, 6). With respect to the development of novel drugs, the effects and side effects of PPAR␦ activators are therefore of great importance.In the last few years, knowledge concerning the impact of PPAR␦ in endothelial cell function has increased. showed that the PPAR␦ agonist L-165041 suppresses C-reactive protein-induced IL-6 expression (10). The expression profile of both cytokines during treatment with various PPAR␦ agonist concentrations in the endothelial quiescent status has yet to be analyzed. Nonetheless, these studies showed that PPAR␦ agonists could suppress the inflammatory processes in activated endothelial cells. The impact of PPAR agonists on the normally quiescent endothelium, however, remains to be elucidated. This could be of significant importance due to the possible broad range of applications of PPAR␦ agonists in various diseases, such as chronic inflammation, glucose metabolism, dyslipidemia, obesity, and cancer therapy, to mention only a small number of possible medical applications.During the process of inflammation, proinflammatory cytokines are produced by various cell types. IL-8 is one of these important cytokines. It is secreted at very low levels from noninduced cells, although the secretion is increased rapidly by a * This work was supported by the Wilhelm Sander Stiftung (M. M.).

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Development of Improved PPARβ/δ Inhibitors

et al. 2011

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GSK0660 (1) is the first peroxisome proliferator-activated receptor (PPAR) β/δ-selective inhibitory ligand described in the literature. Based on its structure, we designed and synthesized a series of modified compounds to establish preliminary structure-activity relationships. Most beneficial for increased binding affinity towards the PPARβ/δ ligand binding domain was the replacement of the 4'-aminophenyl substituent by medium-length n-alkyl chains, such as n-butyl or iso-pentyl. These compounds show activity down to the one-digit nanomolar range, thus possessing up to a tenfold higher binding affinity compared with GSK0660. Additionally, the subtype-specific inhibition of PPARβ/δ was confirmed in a cell-based assay making these compounds invaluable tools for the further exploration of the functions of PPARβ/δ.

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Ligand activation of peroxisome proliferator-activated receptor β/δ (PPARβ/δ) inhibits chemically induced skin tumorigenesis

Cited by 38 publications

References 49 publications

Peroxisome Proliferator-Activated Receptor β/δ Cross Talks with E2F and Attenuates Mitosis in HRAS-Expressing Cells

Peroxisome Proliferator-Activated Receptor β/δ Cross Talks with E2F and Attenuates Mitosis in HRAS-Expressing Cells

Peroxisome Proliferator-activated Receptor δ Activators Induce IL-8 Expression in Nonstimulated Endothelial Cells in a Transcriptional and Posttranscriptional Manner*

Development of Improved PPARβ/δ Inhibitors

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