Use it or lose it: How neurogenesis keeps the brain fit for learning

Shors, Tracey J.; Anderson, Megan L.; Curlik, Daniel M.; Nokia, Miriam S.

doi:10.1016/j.bbr.2011.04.023

Cited by 152 publications

(137 citation statements)

References 107 publications

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“…In particular, hippocampal-dependent learning promotes the survival of newborn cells generated 1 week before training, as a function of task difficulty. Trace eye blink conditioning and spatial learning (reference memory or delayed matching to place) exert a survival-promoting effect (Shors et al, 2012), whereas active shock avoidance and fear contextual memory are insufficient to change cell survival (Pham et al, 2005;Van der Borght et al, 2005;LopezFernandez et al, 2007). More recently, we have discovered that learning-induced survival of these immature neurons depends upon the elimination of youngest newborn cells at a specific developmental period (Drapeau et al, 2007;Dupret et al, 2007;Tronel et al, 2010).…”

Section: Discussionmentioning

confidence: 99%

Long-Lasting Plasticity of Hippocampal Adult-Born Neurons

et al. 2012

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Adult neurogenesis occurs in the dentate gyrus of the hippocampus, which is a key structure in learning and memory. It is believed that adult-born neurons exert their unique role in information processing due to their high plasticity during immature stage that renders them malleable in response to environmental demands. Here, we demonstrate that, in rats, there is no critical time window for experience-induced dendritic plasticity of adult-born neurons as spatial learning in the water maze sculpts the dendritic arbor of adult-born neurons even when they are several months of age. By ablating neurogenesis within a specific period of time, we found that learning was disrupted when the delay between ablation and learning was extended to several months. Together, these results show that mature adult-born neurons are still plastic when they are functionally integrated into dentate network. Our results suggest a new perspective with regard to the role of neo-neurons by highlighting that even mature ones can provide an additional source of plasticity to the brain to process memory information.

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Section: Discussionmentioning

confidence: 99%

Long-Lasting Plasticity of Hippocampal Adult-Born Neurons

et al. 2012

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“…"Use It or Lose It" in Free-Living Mammals Shors et al (2012) have formulated the "use-itor-lose-it" concept for AHN in laboratory rodents, as many behavioral experiments that include some forms of learning increase the survival rates of young cells. Free-living mammals have to cope with a multitude and, in many ways, continually changing stimuli throughout their life.…”

Section: Functional Aspects Of Hippocampal Neurogenesis Variation In mentioning

confidence: 99%

Adult Hippocampal Neurogenesis in Natural Populations of Mammals

Amrein

2015

Cold Spring Harb Perspect Biol

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This review will discuss adult hippocampal neurogenesis in wild mammals of different taxa and outline similarities with and differences from laboratory animals. It begins with a review of evidence for hippocampal neurogenesis in various mammals, and shows the similar patterns of age-dependent decline in cell proliferation in wild and domesticated mammals. In contrast, the pool of immature neurons that originate from proliferative activity varies between species, implying a selective advantage for mammals that can make use of a large number of these functionally special neurons. Furthermore, rapid adaptation of hippocampal neurogenesis to experimental challenges appears to be a characteristic of laboratory rodents. Wild mammals show species-specific, rather stable hippocampal neurogenesis, which appears related to demands that characterize the niche exploited by a species rather than to acute events in the life of its members. Studies that investigate adult neurogenesis in wild mammals are not numerous, but the findings of neurogenesis under natural conditions can provide new insights, and thereby also address the question to which cognitive demands neurogenesis may respond during selection.

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“…For example, the survival of new brain cells is enhanced by spatial navigation learning during Morris water maze tests in rats and mice [reviewed in Shors, 2008;Shors et al, 2012]. Similarly, Hoshooley and Sherry [2007] showed that greater neuron recruitment in the hippocampus is associated with food caching in adult black-capped chickadees, i.e.…”

Section: Introductionmentioning

confidence: 99%

Seasonal Variation in Cell Proliferation and Cell Migration in the Brain of Adult Red-Sided Garter Snakes <b><i>(Thamnophis sirtalis parietalis)</i></b>

2014

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Plasticity in the adult central nervous system has been described in all vertebrate classes as well as in some invertebrate groups. However, the limited taxonomic diversity represented in the current neurogenesis literature limits our ability to assess the functional significance of adult neurogenesis for natural behaviors as well as the evolution of its regulatory mechanisms. In the present study, we used free-ranging red-sided garter snakes (Thamnophis sirtalis parietalis) to test the hypothesis that seasonal shifts in physiology and behavior are associated with seasonal variation in postembryonic neurogenesis. Specifically, we used the thymidine analog 5-bromo-2′-deoxyuridine (BrdU) to determine if the rates of cell proliferation in the adult brain vary between male snakes collected during spring and fall at 1, 5, and 10 days post-BrdU treatment. To assess rates of cell migration within the brain, we further categorized BrdU-labeled cells according to their location within the ventricular zone or parenchymal region. BrdU-labeled cells were localized mainly within the lateral, dorsal, and medial cortex, septal nucleus, nucleus sphericus, preoptic area, and hypothalamus. In all regions, the number of BrdU-labeled cells in the ventricular zone was higher in the fall compared to spring. In the parenchymal region, a significantly higher number of labeled cells was also observed during the fall, but only within the nucleus sphericus and the combined preoptic area/hypothalamus. The immunoreactive cell number did not vary significantly with days post-BrdU treatment in either season or in any brain region. While it is possible that the higher rates of cell proliferation in the fall simply reflect increased growth of all body tissues, including the brain, our data show that seasonal changes in cell migration into the parenchyma are region specific. In red-sided garter snakes and other reptiles, the dorsal and medial cortex is important for spatial navigation and memory, whereas the nucleus sphericus, septal nucleus, and preoptic area/hypothalamus are central to reproductive regulation. Thus, our results provide support for the hypothesis that adult neurogenesis plays a role in mediating seasonal rhythms in migratory and reproductive behaviors.

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Use it or lose it: How neurogenesis keeps the brain fit for learning

Cited by 152 publications

References 107 publications

Long-Lasting Plasticity of Hippocampal Adult-Born Neurons

Long-Lasting Plasticity of Hippocampal Adult-Born Neurons

Adult Hippocampal Neurogenesis in Natural Populations of Mammals

Seasonal Variation in Cell Proliferation and Cell Migration in the Brain of Adult Red-Sided Garter Snakes <b><i>(Thamnophis sirtalis parietalis)</i></b>

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