Regulation of survival in adult hippocampal and glioblastoma stem cell lineages by the homeodomain-only protein HOP

<p>Abstract</p> <p>Background</p> <p>Homeodomain proteins play critical roles in shaping the development of the embryonic central nervous system in mammals. After birth, neurogenic activities are relegated to stem cell niches, which include the subgranular layer of the...

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Main Authors: Altaba Ariel, Epstein Jonathan A, Zbinden Marie, De Toni Arianna, Prochiantz Alain, Caillé Isabelle
Format: Article
Language:English
Published: BMC 2008-05-01
Series:Neural Development
Online Access:http://www.neuraldevelopment.com/content/3/1/13
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spelling doaj-960b27fb0be440daa5a18fa2863f93722020-11-25T00:55:59ZengBMCNeural Development1749-81042008-05-01311310.1186/1749-8104-3-13Regulation of survival in adult hippocampal and glioblastoma stem cell lineages by the homeodomain-only protein HOPAltaba ArielEpstein Jonathan AZbinden MarieDe Toni AriannaProchiantz AlainCaillé Isabelle<p>Abstract</p> <p>Background</p> <p>Homeodomain proteins play critical roles in shaping the development of the embryonic central nervous system in mammals. After birth, neurogenic activities are relegated to stem cell niches, which include the subgranular layer of the dentate gyrus of the hippocampus. Here, we have analyzed the function of HOP (Homeodomain only protein) in this stem cell niche and in human glioblastomas.</p> <p>Results</p> <p>We find that <it>HOP </it>is strongly expressed by radial astrocytes of the dentate gyrus in mice, which are stem cells that give rise to hippocampal granular neurons throughout adulthood. Deletion or down-regulation of <it>HOP </it>results in a decrease of apoptosis of these stem cells without changes in proliferation, and in an increase in the number of newly formed granule neurons. We also find that human glioblastomas largely lack <it>HOP </it>expression and that reintroduction of HOP function in glioma cells cultured as gliomaspheres leads to enhanced apoptosis in a subset of cases. In these cells, HOP function decreases clonogenicity.</p> <p>Conclusion</p> <p>These data suggest that HOP participates in the regulation of the adult mouse hippocampal stem cell niche by negatively affecting cell survival. In addition, HOP may work as a tumor suppressor in a subset of glioblastomas. HOP function thus appears to be critical in the adult brain in a region of continued plasticity, and its deregulation may contribute to disease.</p> http://www.neuraldevelopment.com/content/3/1/13
collection DOAJ
language English
format Article
sources DOAJ
author Altaba Ariel
Epstein Jonathan A
Zbinden Marie
De Toni Arianna
Prochiantz Alain
Caillé Isabelle
spellingShingle Altaba Ariel
Epstein Jonathan A
Zbinden Marie
De Toni Arianna
Prochiantz Alain
Caillé Isabelle
Regulation of survival in adult hippocampal and glioblastoma stem cell lineages by the homeodomain-only protein HOP
Neural Development
author_facet Altaba Ariel
Epstein Jonathan A
Zbinden Marie
De Toni Arianna
Prochiantz Alain
Caillé Isabelle
author_sort Altaba Ariel
title Regulation of survival in adult hippocampal and glioblastoma stem cell lineages by the homeodomain-only protein HOP
title_short Regulation of survival in adult hippocampal and glioblastoma stem cell lineages by the homeodomain-only protein HOP
title_full Regulation of survival in adult hippocampal and glioblastoma stem cell lineages by the homeodomain-only protein HOP
title_fullStr Regulation of survival in adult hippocampal and glioblastoma stem cell lineages by the homeodomain-only protein HOP
title_full_unstemmed Regulation of survival in adult hippocampal and glioblastoma stem cell lineages by the homeodomain-only protein HOP
title_sort regulation of survival in adult hippocampal and glioblastoma stem cell lineages by the homeodomain-only protein hop
publisher BMC
series Neural Development
issn 1749-8104
publishDate 2008-05-01
description <p>Abstract</p> <p>Background</p> <p>Homeodomain proteins play critical roles in shaping the development of the embryonic central nervous system in mammals. After birth, neurogenic activities are relegated to stem cell niches, which include the subgranular layer of the dentate gyrus of the hippocampus. Here, we have analyzed the function of HOP (Homeodomain only protein) in this stem cell niche and in human glioblastomas.</p> <p>Results</p> <p>We find that <it>HOP </it>is strongly expressed by radial astrocytes of the dentate gyrus in mice, which are stem cells that give rise to hippocampal granular neurons throughout adulthood. Deletion or down-regulation of <it>HOP </it>results in a decrease of apoptosis of these stem cells without changes in proliferation, and in an increase in the number of newly formed granule neurons. We also find that human glioblastomas largely lack <it>HOP </it>expression and that reintroduction of HOP function in glioma cells cultured as gliomaspheres leads to enhanced apoptosis in a subset of cases. In these cells, HOP function decreases clonogenicity.</p> <p>Conclusion</p> <p>These data suggest that HOP participates in the regulation of the adult mouse hippocampal stem cell niche by negatively affecting cell survival. In addition, HOP may work as a tumor suppressor in a subset of glioblastomas. HOP function thus appears to be critical in the adult brain in a region of continued plasticity, and its deregulation may contribute to disease.</p>
url http://www.neuraldevelopment.com/content/3/1/13
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