Abstract
BackgroundAdult neurogenesis continuously adds new neurons to the dentate gyrus and the olfactory bulb. It involves the proliferation and subsequent differentiation of neuronal progenitors, and is thus closely linked to the cell cycle machinery. Cell cycle progression is governed by the successive expression, activation and degradation of regulatory proteins. Among them, D-type cyclins control the exit from the G1 phase of the cell cycle. Cyclin D2 (cD2) has been shown to be required for the generation of new neurons in the neurogenic niches of the adult brain. It is differentially expressed during hippocampal development, and adult cD2 knock out (cD2KO) mice virtually lack neurogenesis in the dentate gyrus and olfactory bulb. In the present study we examined the dynamics of postnatal and adult neurogenesis in the dentate gyrus (DG) of cD2KO mice. Animals were injected with bromodeoxyuridine at seven time points during the first 10 months of life and brains were immunohistochemically analyzed for their potential to generate new neurons.ResultsCompared to their WT litters, cD2KO mice had considerably reduced numbers of newly born granule cells during the postnatal period, with neurogenesis becoming virtually absent around postnatal day 28. This was paralleled by a reduction in granule cell numbers, in the volume of the granule cell layer as well as in apoptotic cell death. CD2KO mice did not show any of the age-related changes in neurogenesis and granule cell numbers that were seen in WT litters.ConclusionsThe present study suggests that hippocampal neurogenesis becomes increasingly dependent on cD2 during early postnatal development. In cD2KO mice, hippocampal neurogenesis ceases at a time point at which the tertiary germinative matrix stops proliferating, indicating that cD2 becomes an essential requirement for ongoing neurogenesis with the transition from developmental to adult neurogenesis. Our data further support the notion that adult neurogenesis continuously adds new neurons to the hippocampal network, hence increasing cell density of the DG.
Highlights
Adult neurogenesis continuously adds new neurons to the dentate gyrus and the olfactory bulb
BrdU-positive cell numbers were significantly reduced in the dentate gyrus (DG) of cD2 knock out (cD2KO) mice (p < 0.001), an effect that could be observed at all ages analyzed in this study (Figures 5 and 6)
The difference was lowest at early postnatal ages with about 60% less BrdU-positive cells in cD2KO mice compared to WT litters (P7 and P14, p < 0.002)
Summary
Adult neurogenesis continuously adds new neurons to the dentate gyrus and the olfactory bulb It involves the proliferation and subsequent differentiation of neuronal progenitors, and is closely linked to the cell cycle machinery. Cyclin D2 (cD2) has been shown to be required for the generation of new neurons in the neurogenic niches of the adult brain It is differentially expressed during hippocampal development, and adult cD2 knock out (cD2KO) mice virtually lack neurogenesis in the dentate gyrus and olfactory bulb. As one of the neurogenic zones in the adult mammalian brain, the hippocampal dentate gyrus (DG) generates neural progenitor-derived neurons throughout life This process, known as adult neurogenesis, is modulated by various intrinsic and extrinsic factors ranging from neurotransmitters, growth factors, hormones, physical activity, learning, to seizures and other brain pathologies (reviewed in [1]). D-type cyclins are regarded as constituting a molecular link between the extracellular environment and the cell cycle machinery
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