Conditional ablation and recovery of forebrain neurogenesis in the mouse

Singer, Benjamin H.; Jutkiewicz, Emily M.; Fuller, Cynthia L.; Lichtenwalner, Robin J.; Zhang, Baiyu; Velander, Alan J.; Li, Xiangquan; Gnegy, Margaret E.; Burant, Charles F.; Parent, Jack M.

doi:10.1002/cne.22052

Cited by 60 publications

(54 citation statements)

References 87 publications

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“…To address this question, we have examined LTP in the nestinthymidine kinase (nestin-tk) mouse model, in which herpes simplex virus (HSV) thymidine kinase expression is regulated by the nestin enhancer, enabling the specific and temporally controlled ablation of neurogenesis after the intracerebroventricular administration of ganciclovir (GCV). In this model, treatment with GCV for 28 d results in nearly complete suppression of neurogenesis in youngadult mice (26). Consistent with previous results, we found that LTP was significantly disrupted when assessed immediately following ablation.…”

supporting

confidence: 92%

“…These results suggest that the LTP deficit seen in nestin-tk mice treated with GCV is specific to the loss of newborn DGCs. Recent work suggests that 28 d of GCV treatment in nestin-tk mice results in a loss of newborn DGCs that persists for at least 42 d (6 wk) after the discontinuation of the GCV infusion (26). To determine the impact of persistently suppressed neurogenesis on LTP, experiments similar to those described above (Fig.…”

Section: Resultsmentioning

confidence: 99%

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Compensatory network changes in the dentate gyrus restore long-term potentiation following ablation of neurogenesis in young-adult mice

Singer

Gamelli

Fuller

et al. 2011

Proc. Natl. Acad. Sci. U.S.A.

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It is now well established that neurogenesis in the rodent subgranular zone of the hippocampal dentate gyrus continues throughout adulthood. Neuroblasts born in the dentate subgranular zone migrate into the granule cell layer, where they differentiate into neurons known as dentate granule cells. Suppression of neurogenesis by irradiation or genetic ablation has been shown to disrupt synaptic plasticity in the dentate gyrus and impair some forms of hippocampus-dependent learning and memory. Using a recently developed transgenic mouse model for suppressing neurogenesis, we sought to determine the long-term impact of ablating neurogenesis on synaptic plasticity in young-adult mice. Consistent with previous reports, we found that ablation of neurogenesis resulted in significant deficits in dentate gyrus long-term potentiation (LTP) when examined at a time proximal to the ablation. However, the observed deficits in LTP were not permanent. LTP in the dentate gyrus was restored within 6 wk and this recovery occurred in the complete absence of neurogenesis. The recovery in LTP was accompanied by prominent changes within the dentate gyrus, including an increase in the survival rate of newborn cells that were proliferating just before the ablation and a reduction in inhibitory input to the granule cells of the dentate gyrus. These findings suggest that prolonged suppression of neurogenesis in young-adult mice results in wide-ranging compensatory changes in the structure and dynamics of the dentate gyrus that function to restore plasticity.adult neurogenesis | thymidine kinase | metaplasticity | miniature inhibitory postsynaptic currents F orebrain neurogenesis persists into adulthood in the subgranular zone (SGZ) of the hippocampal dentate gyrus in rodents (1-4). Under normal conditions (i.e., in the absence of overt pathology) neuroblasts that arise in the SGZ migrate a short distance into the dentate granule cell layer (GCL) and differentiate into dentate granule cells (DGCs), where they subsequently reach functional maturity (5, 6). The birth, integration, and survival of DGCs are modulated by environmental enrichment (7), exercise (8), stress (9, 10), hippocampus-dependent learning (11), and direct manipulation of neuronal activity (12, 13). In addition, adult-born DGCs respond preferentially in hippocampus-dependent memory tasks (14) and display increased synaptic plasticity relative to mature DGCs (15,16).The correlation of increased DGC neurogenesis with cognitively demanding tasks has led to the hypothesis that adult-born neurons are integral participants in hippocampus-dependent memory processing and behavior. The role of adult-born DGCs in hippocampal function has been studied at the behavioral level in rodents after suppressing neurogenesis with antimitotic agents (17, 18), radiation (19), or genetic targeting (19)(20)(21)(22). These studies indicate that adult-born DGCs are necessary for some hippocampus-dependent tasks, although results have been inconsistent and vary by rodent species and strain, behavioral ...

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supporting

confidence: 92%

Section: Resultsmentioning

confidence: 99%

Compensatory network changes in the dentate gyrus restore long-term potentiation following ablation of neurogenesis in young-adult mice

Singer

Gamelli

Fuller

et al. 2011

Proc. Natl. Acad. Sci. U.S.A.

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“…Expression of TK renders the cell population of interest susceptible to the cytotoxic effect of GCV (36). Studies to date have used either GFAP (20)(21)(22) or nestin (23) to direct the expression of TK. GFAP is a type III intermediate filament protein expressed classically in astrocytes, including SVZ astrocytes that give rise to neurons (37) and oligodendrocytes (38).…”

Section: Resultsmentioning

confidence: 99%

“…Several techniques have been used for this purpose, including x-irradiation (7)(8)(9)(10)(11)(12)(13), antimitotic (4,(14)(15)(16)(17)(18) or other antiproliferative (19) drugs, and conditional transgenic targeting of selected [glial fibrillary acidic protein (GFAP)-, nestin-, or homolog of Drosophila taillessexpressing] cell populations with HSV-1 thymidine kinase (TK) (20)(21)(22)(23) or inducible recombination (24). However, studies that use these ablation techniques to assess the functional significance of neurogenesis can be difficult to interpret, because ablation may be accompanied by inflammatory responses with microglial activation (7), alterations in microvascular anatomy (7), systemic toxicity (18), or involvement of nonneuronal cell lineages (25).…”

mentioning

confidence: 99%

Transgenic ablation of doublecortin-expressing cells suppresses adult neurogenesis and worsens stroke outcome in mice

Jin

Wang²,

Xie³

et al. 2010

Proc. Natl. Acad. Sci. U.S.A.

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166

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Injury stimulates neurogenesis in the adult brain, but the role of injury-induced neurogenesis in brain repair and recovery is uncertain. One strategy for investigating this issue is to ablate neuronal precursors and thereby prevent neurogenesis, but this is difficult to achieve in a specific fashion. We produced transgenic mice that express herpes simplex virus thymidine kinase (TK) under control of the promoter for doublecortin (Dcx), a microtubuleassociated protein expressed in newborn and migrating neurons. Treatment for 14 days with the antiviral drug ganciclovir (GCV) depleted Dcx-expressing and BrdU-labeled cells from the rostral subventricular zone and dentate gyrus, and abolished neurogenesis and associated neuromigration induced by focal cerebral ischemia. GCV treatment of Dcx-TK transgenic, but not WT, mice also increased infarct size and exacerbated postischemic sensorimotor behavioral deficits measured by rotarod, limb placing, and elevated body swing tests. These findings provide evidence that injuryinduced neurogenesis contributes to stroke outcome and might therefore be a target for stroke therapy.T he finding that brain injury stimulates the production of new neurons (neurogenesis) in the mammalian brain (1) suggests a role for this process in brain repair. Injury-induced neurogenesis is observed across a broad range of injury models in experimental animals and human patients. Focal brain ischemia, for example, triggers increased proliferation of neuronal precursor cells in the anterior subventricular zone (SVZ), followed by their migration into ischemic brain regions, where they differentiate and mature (2-6). This raises the possibility that therapeutic enhancement of injury-induced neurogenesis might constitute a new approach to the treatment of stroke or related disorders.One strategy for investigating the contribution of adult neurogenesis to brain function or repair is to ablate neuronal precursors in the brain's principal neuroproliferative zones-the anterior SVZ and the hippocampal dentate gyrus (DG). Several techniques have been used for this purpose, including x-irradiation (7-13), antimitotic (4, 14-18) or other antiproliferative (19) drugs, and conditional transgenic targeting of selected [glial fibrillary acidic protein (GFAP)-, nestin-, or homolog of Drosophila taillessexpressing] cell populations with HSV-1 thymidine kinase (TK) (20-23) or inducible recombination (24). However, studies that use these ablation techniques to assess the functional significance of neurogenesis can be difficult to interpret, because ablation may be accompanied by inflammatory responses with microglial activation (7), alterations in microvascular anatomy (7), systemic toxicity (18), or involvement of nonneuronal cell lineages (25).We report the results of studies on the effects of neuronal precursor cell depletion on outcome from experimental stroke in transgenic mice that express TK under control of the doublecortin (Dcx) promoter (26). Dcx is a microtubule-associated protein expressed primarily in mig...

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“…Indeed, it was shown that animals with blocked adult neurogenesis do not recover from depressionlike behavior when chronically administered with ADs (Santarelli et al, 2003;Surget et al, 2008;David et al, 2009;Onksen et al, 2011;Perera et al, 2011). However, recent studies suggest both neurogenesis-dependent and independent mechanisms underlying ADs action, as more studies show none or only partial effect of reducing neurogenesis on restoration of behavioral homeostasis by ADs (Meshi et al, 2006;David et al, 2007;Holick et al, 2008;Surget et al, 2008;Bessa et al, 2009a;David et al, 2009;Singer et al, 2009;Nollet et al, 2012).…”

Section: Introductionmentioning

confidence: 99%

Mice with ablated adult brain neurogenesis are not impaired in antidepressant response to chronic fluoxetine

Jedynak

Kos

Sandi

et al. 2014

Journal of Psychiatric Research

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a b s t r a c tThe neurogenesis hypothesis of major depression has two main facets. One states that the illness results from decreased neurogenesis while the other claims that the very functioning of antidepressants depends on increased neurogenesis. In order to verify the latter, we have used cyclin D2 knockout mice (cD2 KO mice), known to have virtually no adult brain neurogenesis, and we demonstrate that these mice successfully respond to chronic fluoxetine. After unpredictable chronic mild stress, mutant mice showed depression-like behavior in forced swim test, which was eliminated with chronic fluoxetine treatment, despite its lack of impact on adult hippocampal neurogenesis in cD2 KO mice. Our results suggest that new neurons are not indispensable for the action of antidepressants such as fluoxetine. Using forced swim test and tail suspension test, we also did not observe depression-like behavior in control cD2 KO mice, which argues against the link between decreased adult brain neurogenesis and major depression.

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Conditional ablation and recovery of forebrain neurogenesis in the mouse

Cited by 60 publications

References 87 publications

Compensatory network changes in the dentate gyrus restore long-term potentiation following ablation of neurogenesis in young-adult mice

Compensatory network changes in the dentate gyrus restore long-term potentiation following ablation of neurogenesis in young-adult mice

Transgenic ablation of doublecortin-expressing cells suppresses adult neurogenesis and worsens stroke outcome in mice

Mice with ablated adult brain neurogenesis are not impaired in antidepressant response to chronic fluoxetine

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