Literature DB >> 23105093

Peroxisome proliferator-activated receptor-γ activation enhances insulin-stimulated glucose disposal by reducing ped/pea-15 gene expression in skeletal muscle cells: evidence for involvement of activator protein-1.

Paola Ungaro1, Paola Mirra, Francesco Oriente, Cecilia Nigro, Marco Ciccarelli, Viviana Vastolo, Michele Longo, Giuseppe Perruolo, Rosa Spinelli, Pietro Formisano, Claudia Miele, Francesco Beguinot.   

Abstract

The gene network responsible for inflammation-induced insulin resistance remains enigmatic. In this study, we show that, in L6 cells, rosiglitazone- as well as pioglitazone-dependent activation of peroxisome proliferator-activated receptor-γ (PPARγ) represses transcription of the ped/pea-15 gene, whose increased activity impairs glucose tolerance in mice and humans. Rosiglitazone enhanced insulin-induced glucose uptake in L6 cells expressing the endogenous ped/pea-15 gene but not in cells expressing ped/pea-15 under the control of an exogenous promoter. The ability of PPARγ to affect ped/pea-15 expression was also lost in cells and in C57BL/6J transgenic mice expressing ped/pea-15 under the control of an exogenous promoter, suggesting that ped/pea-15 repression may contribute to rosiglitazone action on glucose disposal. Indeed, high fat diet mice showed insulin resistance and increased ped/pea-15 levels, although these effects were reduced by rosiglitazone treatment. Both supershift and ChIP assays revealed the presence of the AP-1 component c-JUN at the PED/PEA-15 promoter upon 12-O-tetradecanoylphorbol-13-acetate stimulation of the cells. In these experiments, rosiglitazone treatment reduced c-JUN presence at the PED/PEA-15 promoter. This effect was not associated with a decrease in c-JUN expression. In addition, c-jun silencing in L6 cells lowered ped/pea-15 expression and caused nonresponsiveness to rosiglitazone, although c-jun overexpression enhanced the binding to the ped/pea-15 promoter and blocked the rosiglitazone effect. These results indicate that PPARγ regulates ped/pea-15 transcription by inhibiting c-JUN binding at the ped/pea-15 promoter. Thus, ped/pea-15 is downstream of a major PPARγ-regulated inflammatory network. Repression of ped/pea-15 transcription might contribute to the PPARγ regulation of muscle sensitivity to insulin.

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Year:  2012        PMID: 23105093      PMCID: PMC3522290          DOI: 10.1074/jbc.M112.406637

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  44 in total

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Review 3.  The cellular and signaling networks linking the immune system and metabolism in disease.

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4.  Amino acid and insulin signaling via the mTOR/p70 S6 kinase pathway. A negative feedback mechanism leading to insulin resistance in skeletal muscle cells.

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6.  Molecular cloning and characterization of the human PED/PEA-15 gene promoter reveal antagonistic regulation by hepatocyte nuclear factor 4alpha and chicken ovalbumin upstream promoter transcription factor II.

Authors:  Paola Ungaro; Raffaele Teperino; Paola Mirra; Angela Cassese; Francesca Fiory; Giuseppe Perruolo; Claudia Miele; Markku Laakso; Pietro Formisano; Francesco Beguinot
Journal:  J Biol Chem       Date:  2008-09-02       Impact factor: 5.157

7.  Muscle-specific Pparg deletion causes insulin resistance.

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Journal:  J Biol Chem       Date:  2002-01-14       Impact factor: 5.157

9.  Protein kinase C (PKC)-alpha activation inhibits PKC-zeta and mediates the action of PED/PEA-15 on glucose transport in the L6 skeletal muscle cells.

Authors:  G Condorelli; G Vigliotta; A Trencia; M A Maitan; M Caruso; C Miele; F Oriente; S Santopietro; P Formisano; F Beguinot
Journal:  Diabetes       Date:  2001-06       Impact factor: 9.461

10.  Differential effects of calorie restriction and exercise on the adipose transcriptome in diet-induced obese mice.

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  6 in total

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2.  Glucose-induced expression of the homeotic transcription factor Prep1 is associated with histone post-translational modifications in skeletal muscle.

Authors:  Marco Ciccarelli; Viviana Vastolo; Luigi Albano; Manuela Lecce; Serena Cabaro; Antonietta Liotti; Michele Longo; Francesco Oriente; Gian Luigi Russo; Paolo Emidio Macchia; Pietro Formisano; Francesco Beguinot; Paola Ungaro
Journal:  Diabetologia       Date:  2015-10-09       Impact factor: 10.122

Review 3.  Molecular basis of ageing in chronic metabolic diseases.

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4.  ZMAT3 hypomethylation contributes to early senescence of preadipocytes from healthy first-degree relatives of type 2 diabetics.

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Journal:  Aging Cell       Date:  2022-02-11       Impact factor: 11.005

5.  Adenoviral gene transfer of PLD1-D4 enhances insulin sensitivity in mice by disrupting phospholipase D1 interaction with PED/PEA-15.

Authors:  Angela Cassese; Gregory A Raciti; Francesca Fiory; Cecilia Nigro; Luca Ulianich; Ilenia Castanò; Vittoria D'Esposito; Daniela Terracciano; Lucio Pastore; Pietro Formisano; Francesco Beguinot; Claudia Miele
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Review 6.  Phosphoprotein enriched in astrocytes (PEA)-15: a potential therapeutic target in multiple disease states.

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  6 in total

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