Estradiol Activates β-Catenin Dependent Transcription in Neurons

Estradiol may fulfill a plethora of functions in neurons, in which much of its activity is associated with its capacity to directly bind and dimerize estrogen receptors. This hormone-protein complex can either bind directly to estrogen response elements (ERE's) in gene promoters, or it may act...

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Autores principales: Varea, Olga, Garrido, Juan Jose, Dopazo, Ana, Mendez, Pablo, Garcia-Segura, Luis Miguel, Wandosell, Francisco
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2009
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2664482/
https://www.ncbi.nlm.nih.gov/pubmed/19360103
http://dx.doi.org/10.1371/journal.pone.0005153
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author Varea, Olga
Garrido, Juan Jose
Dopazo, Ana
Mendez, Pablo
Garcia-Segura, Luis Miguel
Wandosell, Francisco
author_facet Varea, Olga
Garrido, Juan Jose
Dopazo, Ana
Mendez, Pablo
Garcia-Segura, Luis Miguel
Wandosell, Francisco
author_sort Varea, Olga
collection PubMed
description Estradiol may fulfill a plethora of functions in neurons, in which much of its activity is associated with its capacity to directly bind and dimerize estrogen receptors. This hormone-protein complex can either bind directly to estrogen response elements (ERE's) in gene promoters, or it may act as a cofactor at non-ERE sites interacting with other DNA-binding elements such as AP-1 or c-Jun. Many of the neuroprotective effects described for estrogen have been associated with this mode of action. However, recent evidence suggests that in addition to these “genomic effects”, estrogen may also act as a more general “trophic factor” triggering cytoplasmic signals and extending the potential activity of this hormone. We demonstrated that estrogen receptor alpha associates with β-catenin and glycogen synthase kinase 3 in the brain and in neurons, which has since been confirmed by others. Here, we show that the action of estradiol activates β-catenin transcription in neuroblastoma cells and in primary cortical neurons. This activation is time and concentration-dependent, and it may be abolished by the estrogen receptor antagonist ICI 182780. The transcriptional activation of β-catenin is dependent on lymphoid enhancer binding factor-1 (LEF-1) and a truncated-mutant of LEF-1 almost completely blocks estradiol TCF-mediated transcription. Transcription of a TCF-reporter in a transgenic mouse model is enhanced by estradiol in a similar fashion to that produced by Wnt3a. In addition, activation of a luciferase reporter driven by the engrailed promoter with three LEF-1 repeats was mediated by estradiol. We established a cell line that constitutively expresses a dominant-negative LEF-1 and it was used in a gene expression microarray analysis. In this way, genes that respond to estradiol or Wnt3a, sensitive to LEF-1, could be identified and validated. Together, these data demonstrate the existence of a new signaling pathway controlled by estradiol in neurons. This pathway shares some elements of the insulin-like growth factor-1/Insulin and Wnt signaling pathways, however, our data strongly suggest that it is different from that of both these ligands. These findings may reveal a set of new physiological roles for estrogens, at least in the Central Nervous System (CNS).
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spelling pubmed-26644822009-04-10 Estradiol Activates β-Catenin Dependent Transcription in Neurons Varea, Olga Garrido, Juan Jose Dopazo, Ana Mendez, Pablo Garcia-Segura, Luis Miguel Wandosell, Francisco PLoS One Research Article Estradiol may fulfill a plethora of functions in neurons, in which much of its activity is associated with its capacity to directly bind and dimerize estrogen receptors. This hormone-protein complex can either bind directly to estrogen response elements (ERE's) in gene promoters, or it may act as a cofactor at non-ERE sites interacting with other DNA-binding elements such as AP-1 or c-Jun. Many of the neuroprotective effects described for estrogen have been associated with this mode of action. However, recent evidence suggests that in addition to these “genomic effects”, estrogen may also act as a more general “trophic factor” triggering cytoplasmic signals and extending the potential activity of this hormone. We demonstrated that estrogen receptor alpha associates with β-catenin and glycogen synthase kinase 3 in the brain and in neurons, which has since been confirmed by others. Here, we show that the action of estradiol activates β-catenin transcription in neuroblastoma cells and in primary cortical neurons. This activation is time and concentration-dependent, and it may be abolished by the estrogen receptor antagonist ICI 182780. The transcriptional activation of β-catenin is dependent on lymphoid enhancer binding factor-1 (LEF-1) and a truncated-mutant of LEF-1 almost completely blocks estradiol TCF-mediated transcription. Transcription of a TCF-reporter in a transgenic mouse model is enhanced by estradiol in a similar fashion to that produced by Wnt3a. In addition, activation of a luciferase reporter driven by the engrailed promoter with three LEF-1 repeats was mediated by estradiol. We established a cell line that constitutively expresses a dominant-negative LEF-1 and it was used in a gene expression microarray analysis. In this way, genes that respond to estradiol or Wnt3a, sensitive to LEF-1, could be identified and validated. Together, these data demonstrate the existence of a new signaling pathway controlled by estradiol in neurons. This pathway shares some elements of the insulin-like growth factor-1/Insulin and Wnt signaling pathways, however, our data strongly suggest that it is different from that of both these ligands. These findings may reveal a set of new physiological roles for estrogens, at least in the Central Nervous System (CNS). Public Library of Science 2009-04-10 /pmc/articles/PMC2664482/ /pubmed/19360103 http://dx.doi.org/10.1371/journal.pone.0005153 Text en Varea 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
Varea, Olga
Garrido, Juan Jose
Dopazo, Ana
Mendez, Pablo
Garcia-Segura, Luis Miguel
Wandosell, Francisco
Estradiol Activates β-Catenin Dependent Transcription in Neurons
title Estradiol Activates β-Catenin Dependent Transcription in Neurons
title_full Estradiol Activates β-Catenin Dependent Transcription in Neurons
title_fullStr Estradiol Activates β-Catenin Dependent Transcription in Neurons
title_full_unstemmed Estradiol Activates β-Catenin Dependent Transcription in Neurons
title_short Estradiol Activates β-Catenin Dependent Transcription in Neurons
title_sort estradiol activates β-catenin dependent transcription in neurons
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2664482/
https://www.ncbi.nlm.nih.gov/pubmed/19360103
http://dx.doi.org/10.1371/journal.pone.0005153
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AT dopazoana estradiolactivatesbcatenindependenttranscriptioninneurons
AT mendezpablo estradiolactivatesbcatenindependenttranscriptioninneurons
AT garciaseguraluismiguel estradiolactivatesbcatenindependenttranscriptioninneurons
AT wandosellfrancisco estradiolactivatesbcatenindependenttranscriptioninneurons

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