PPAR beta/delta and PPAR gamma maintain undifferentiated phenotypes of mouse adult neural precursor cells from the subventricular zone
Author
dc.contributor.author
Bernal, Carolina
Author
dc.contributor.author
Araya, Claudia
Author
dc.contributor.author
Palma Alvarado, Verónica
Author
dc.contributor.author
Bronfman, Miguel
Admission date
dc.date.accessioned
2015-08-23T00:49:53Z
Available date
dc.date.available
2015-08-23T00:49:53Z
Publication date
dc.date.issued
2015
Cita de ítem
dc.identifier.citation
Frontiers in Cellular Neuroscience March 2015 Volume 9 Article 78
en_US
Identifier
dc.identifier.issn
1662-5102
Identifier
dc.identifier.other
10.3389/fncel.2015.00078
Identifier
dc.identifier.uri
https://repositorio.uchile.cl/handle/2250/133054
Abstract
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The subventricular zone (SVZ) is one of the main niches of neural stem cells in the adult mammalian brain. Stem and precursor cells in this region are the source for neurogenesis and oligodendrogesis, mainly in the olfactory bulb and corpus callosum, respectively. The identification of the molecular components regulating the decision of these cells to differentiate or maintain an undifferentiated state is important in order to understand the modulation of neurogenic processes in physiological and pathological conditions. PPARs are a group of transcription factors, activated by lipid ligands, with important functions in cellular differentiation and proliferation in several tissues. In this work, we demonstrate that mouse adult neural precursor cells (NPCs), in situ and in vitro, express PPAR beta/delta and PPAR gamma. Pharmacological activation of both PPARs isoforms induces proliferation and maintenance of the undifferentiated phenotype. Congruently, inhibition of PPAR beta/delta and PPAR gamma results in a decrease of proliferation and loss of the undifferentiated phenotype. Interestingly, PPAR gamma regulates the level of EGFR in adult NPCs, concurrent with it is function described in embryonic NPCs. Furthermore, we describe for the first time that PPAR beta/delta regulates SOX2 level in adult NPCs, probably through a direct transcriptional regulation, as we identified two putative PPAR response elements in the promoter region of Sox2. EGFR and SOX2 are key players in neural stem/precursor cells self-renewal. Finally, rosiglitazone, a PPAR gamma ligand, increases PPAR beta/delta level, suggesting a possible cooperation between these two PPARs in the control of cell fate behavior. Our work contributes to the understanding of the molecular mechanisms associated to neural cell fate decision and places PPAR beta/delta and PPAR gamma as interesting new targets of modulation of mammalian brain homeostasis.