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An Ebox Element in the Proximal Gata4 Promoter Is Required for Gata4 Expression In Vivo

GATA4 is an essential transcription factor required for the development and function of multiple tissues, including a major role in gonadogenesis. Despite its crucial role, the molecular mechanisms that regulate Gata4 expression in vivo remain poorly understood. We recently found that the Gata4 gene...

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Autores principales: Boulende Sab, Alain, Bouchard, Marie-France, Béland, Mélanie, Prud'homme, Bruno, Souchkova, Ouliana, Viger, Robert S., Pilon, Nicolas
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2011
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3236771/
https://www.ncbi.nlm.nih.gov/pubmed/22174950
http://dx.doi.org/10.1371/journal.pone.0029038
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author Boulende Sab, Alain
Bouchard, Marie-France
Béland, Mélanie
Prud'homme, Bruno
Souchkova, Ouliana
Viger, Robert S.
Pilon, Nicolas
author_facet Boulende Sab, Alain
Bouchard, Marie-France
Béland, Mélanie
Prud'homme, Bruno
Souchkova, Ouliana
Viger, Robert S.
Pilon, Nicolas
author_sort Boulende Sab, Alain
collection PubMed
description GATA4 is an essential transcription factor required for the development and function of multiple tissues, including a major role in gonadogenesis. Despite its crucial role, the molecular mechanisms that regulate Gata4 expression in vivo remain poorly understood. We recently found that the Gata4 gene is expressed as multiple transcripts with distinct 5′ origins. These co-expressed alternative transcripts are generated by different non-coding first exons with transcripts E1a and E1b being the most prominent. Moreover, we previously showed that an Ebox element, located in Gata4 5′ flanking sequences upstream of exon 1a, is important for the promoter activity of these sequences in cell lines. To confirm the importance of this element in vivo, we generated and characterized Gata4 Ebox knockout mice. Quantitative PCR analyses realized on gonads, heart and liver at three developmental stages (embryonic, pre-pubertal and adult) revealed that the Ebox mutation leads to a robust and specific decrease (up to 89%) of Gata4 E1a transcript expression in all tissues and stages examined. However, a detailed characterization of the gonads revealed normal morphology and GATA4 protein levels in these mutants. Our qPCR data further indicate that this outcome is most likely due to the presence of Gata4 E1b mRNA, whose expression levels were not decreased by the Ebox mutation. In conclusion, our work clearly confirms the importance of the proximal Ebox element and suggests that adequate GATA4 protein expression is likely protected by a compensation mechanism between Gata4 E1a and E1b transcripts operating at the translational level.
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spelling pubmed-32367712011-12-15 An Ebox Element in the Proximal Gata4 Promoter Is Required for Gata4 Expression In Vivo Boulende Sab, Alain Bouchard, Marie-France Béland, Mélanie Prud'homme, Bruno Souchkova, Ouliana Viger, Robert S. Pilon, Nicolas PLoS One Research Article GATA4 is an essential transcription factor required for the development and function of multiple tissues, including a major role in gonadogenesis. Despite its crucial role, the molecular mechanisms that regulate Gata4 expression in vivo remain poorly understood. We recently found that the Gata4 gene is expressed as multiple transcripts with distinct 5′ origins. These co-expressed alternative transcripts are generated by different non-coding first exons with transcripts E1a and E1b being the most prominent. Moreover, we previously showed that an Ebox element, located in Gata4 5′ flanking sequences upstream of exon 1a, is important for the promoter activity of these sequences in cell lines. To confirm the importance of this element in vivo, we generated and characterized Gata4 Ebox knockout mice. Quantitative PCR analyses realized on gonads, heart and liver at three developmental stages (embryonic, pre-pubertal and adult) revealed that the Ebox mutation leads to a robust and specific decrease (up to 89%) of Gata4 E1a transcript expression in all tissues and stages examined. However, a detailed characterization of the gonads revealed normal morphology and GATA4 protein levels in these mutants. Our qPCR data further indicate that this outcome is most likely due to the presence of Gata4 E1b mRNA, whose expression levels were not decreased by the Ebox mutation. In conclusion, our work clearly confirms the importance of the proximal Ebox element and suggests that adequate GATA4 protein expression is likely protected by a compensation mechanism between Gata4 E1a and E1b transcripts operating at the translational level. Public Library of Science 2011-12-13 /pmc/articles/PMC3236771/ /pubmed/22174950 http://dx.doi.org/10.1371/journal.pone.0029038 Text en Boulende Sab et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Boulende Sab, Alain
Bouchard, Marie-France
Béland, Mélanie
Prud'homme, Bruno
Souchkova, Ouliana
Viger, Robert S.
Pilon, Nicolas
An Ebox Element in the Proximal Gata4 Promoter Is Required for Gata4 Expression In Vivo
title An Ebox Element in the Proximal Gata4 Promoter Is Required for Gata4 Expression In Vivo
title_full An Ebox Element in the Proximal Gata4 Promoter Is Required for Gata4 Expression In Vivo
title_fullStr An Ebox Element in the Proximal Gata4 Promoter Is Required for Gata4 Expression In Vivo
title_full_unstemmed An Ebox Element in the Proximal Gata4 Promoter Is Required for Gata4 Expression In Vivo
title_short An Ebox Element in the Proximal Gata4 Promoter Is Required for Gata4 Expression In Vivo
title_sort ebox element in the proximal gata4 promoter is required for gata4 expression in vivo
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3236771/
https://www.ncbi.nlm.nih.gov/pubmed/22174950
http://dx.doi.org/10.1371/journal.pone.0029038
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