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PPARG in Human Adipogenesis: Differential Contribution of Canonical Transcripts and Dominant Negative Isoforms
by
F. Beguinot
, M. Aprile
, P. Formisano
, A. Ciccodicola
, V. D'Esposito
, M. R. Ambrosio
, V. Costa
in
Adipocytes
/ Cell culture
/ Diabetes
/ Genes
/ Genetic variation
/ Health aspects
/ Identification and classification
/ Ligands
/ Metabolism
/ Proteins
/ Rodents
/ Studies
/ Transcription factors
2014
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PPARG in Human Adipogenesis: Differential Contribution of Canonical Transcripts and Dominant Negative Isoforms
by
F. Beguinot
, M. Aprile
, P. Formisano
, A. Ciccodicola
, V. D'Esposito
, M. R. Ambrosio
, V. Costa
in
Adipocytes
/ Cell culture
/ Diabetes
/ Genes
/ Genetic variation
/ Health aspects
/ Identification and classification
/ Ligands
/ Metabolism
/ Proteins
/ Rodents
/ Studies
/ Transcription factors
2014
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While trying to remove the title from your shelf something went wrong :( Kindly try again later!
Do you wish to request the book?
PPARG in Human Adipogenesis: Differential Contribution of Canonical Transcripts and Dominant Negative Isoforms
by
F. Beguinot
, M. Aprile
, P. Formisano
, A. Ciccodicola
, V. D'Esposito
, M. R. Ambrosio
, V. Costa
in
Adipocytes
/ Cell culture
/ Diabetes
/ Genes
/ Genetic variation
/ Health aspects
/ Identification and classification
/ Ligands
/ Metabolism
/ Proteins
/ Rodents
/ Studies
/ Transcription factors
2014
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PPARG in Human Adipogenesis: Differential Contribution of Canonical Transcripts and Dominant Negative Isoforms
Journal Article
PPARG in Human Adipogenesis: Differential Contribution of Canonical Transcripts and Dominant Negative Isoforms
2014
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Overview
The nuclear receptor PPARγ is a key regulator of adipogenesis, and alterations of its function are associated with different pathological processes related to metabolic syndrome. We recently identified two PPARG transcripts encoding dominant negative PPARγ isoforms. The existence of different PPARG variants suggests that alternative splicing is crucial to modulate PPARγ function, underlying some underestimated aspects of its regulation. Here we investigate PPARG expression in different tissues and cells affected in metabolic syndrome and, in particular, during adipocyte differentiation of human mesenchymal stem cells. We defined the transcript-specific expression pattern of PPARG variants encoding both canonical and dominant negative isoforms and identified a novel PPARG transcript, γ1ORF4. Our analysis indicated that, during adipogenesis, the transcription of alternative PPARG variants is regulated in a time-specific manner through differential usage of distinct promoters. In addition, our analysis describes—for the first time—the differential contribution of three ORF4 variants to this process, suggesting a still unexplored role for these dominant negative isoforms during adipogenesis. Therefore, our results highlight crucial aspects of PPARG regulation, suggesting the need of further investigation to rule out the differential impact of all PPARG transcripts in both physiologic and pathologic conditions, such as metabolism-related disorders.
Publisher
Hindawi Limiteds,Hindawi Publishing Corporation,John Wiley & Sons, Inc,Hindawi Limited,Wiley
Subject
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