Literature DB >> 23554226

In vivo contribution of nestin- and GLAST-lineage cells to adult hippocampal neurogenesis.

Nathan A DeCarolis1, Maxwell Mechanic, David Petrik, Adam Carlton, Jessica L Ables, Shveta Malhotra, Robert Bachoo, Magdalena Götz, Diane C Lagace, Amelia J Eisch.   

Abstract

Radial glia-like cells (RGCs) are the hypothesized source of adult hippocampal neurogenesis. However, the current model of hippocampal neurogenesis does not fully incorporate the in vivo heterogeneity of RGCs. In order to better understand the contribution of different RGC subtypes to adult hippocampal neurogenesis, we employed widely used transgenic lines (Nestin-CreER(T2) and GLAST::CreER(T2) mice) to explore how RGCs contribute to neurogenesis under basal conditions and after stimulation and depletion of neural progenitor cells. We first used these inducible fate-tracking transgenic lines to define the similarities and differences in the contribution of nestin- and GLAST-lineage cells to basal long-term hippocampal neurogenesis. We then explored the ability of nestin- and GLAST-lineage RGCs to contribute to neurogenesis after experimental manipulations that either ablate neurogenesis (i.c.v. application of the anti-mitotic AraC, cytosine-β-D-arabinofuranoside) or stimulate neurogenesis (wheel running). Interestingly, in both ablation and stimulation experiments, labeled RGCs in GLAST::CreER(T2) mice appear to contribute to neurogenesis, whereas RGCs in Nestin-CreER(T2) mice do not. Finally, using NestinGFP reporter mice, we expanded on previous research by showing that not all RGCs in the adult dentate gyrus subgranular zone express nestin, and therefore RGCs are antigenically heterogeneous. These findings are important for the field, as they allow appropriately conservative interpretation of existing and future data that emerge from these inducible transgenic lines. These findings also raise important questions about the differences between transgenic driver lines, the heterogeneity of RGCs, and the potential differences in progenitor cell behavior between transgenic lines. As these findings highlight the possible differences in the contribution of cells to long-term neurogenesis in vivo, they indicate that the current models of hippocampal neurogenesis should be modified to include RGC lineage heterogeneity.
Copyright © 2013 Wiley Periodicals, Inc.

Entities:  

Keywords:  Cre recombinase; dentate gyrus; genetic fate tracking; radial glial cell; subgranular zone

Mesh:

Substances:

Year:  2013        PMID: 23554226      PMCID: PMC3732558          DOI: 10.1002/hipo.22130

Source DB:  PubMed          Journal:  Hippocampus        ISSN: 1050-9631            Impact factor:   3.899


  39 in total

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Authors:  Todd E Anthony; Corinna Klein; Gord Fishell; Nathaniel Heintz
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4.  Mosaic organization of neural stem cells in the adult brain.

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Review 1.  Viral and transgenic reporters and genetic analysis of adult neurogenesis.

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3.  Distinct determinants of sparse activation during granule cell maturation.

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4.  Adult hippocampal neural stem and progenitor cells regulate the neurogenic niche by secreting VEGF.

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7.  Transgenic mouse models for studying adult neurogenesis.

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8.  Acute and fractionated exposure to high-LET (56)Fe HZE-particle radiation both result in similar long-term deficits in adult hippocampal neurogenesis.

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9.  Adult Neurogenesis Is Sustained by Symmetric Self-Renewal and Differentiation.

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10.  Prospective identification and purification of quiescent adult neural stem cells from their in vivo niche.

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