4.7 Article

Neural stem cells in the adult olfactory bulb core generate mature neurons in vivo

期刊

STEM CELLS
卷 39, 期 9, 页码 1253-1269

出版社

OXFORD UNIV PRESS
DOI: 10.1002/stem.3393

关键词

adult neurogenesis; calretinin; interneurons; neural stem cells; olfactory bulb; synapses

资金

  1. Comunidad de Madrid [S2011/BMD-2336]
  2. Consejo Superior de Investigaciones Cientificas [201220E098, 201320E054]
  3. Generalitat Valenciana [PROMETEO/2018/055]
  4. Instituto de Salud Carlos III [CIBERNED CB06/05/0065, RD16/0011/0024, PIE14/00061]
  5. Secretaria de Estado de Investigacion, Desarrollo e Innovacion [BFU2016-80870-P, SAF2013-4759R, SAF2016-80419-R, PID2019-109059RB-I00, SAF2015-70433-R]

向作者/读者索取更多资源

In this study, injected EGFP-labeled retroviral particles in the adult olfactory bulb core of mice revealed that NSCs could generate multipotent neurons and glial cells. These newly generated neurons were able to establish synaptic contacts and be integrated into the olfactory bulb circuits.
Although previous studies suggest that neural stem cells (NSCs) exist in the adult olfactory bulb (OB), their location, identity, and capacity to generate mature neurons in vivo has been little explored. Here, we injected enhanced green fluorescent protein (EGFP)-expressing retroviral particles into the OB core of adult mice to label dividing cells and to track the differentiation/maturation of any neurons they might generate. EGFP-labeled cells initially expressed adult NSC markers on days 1 to 3 postinjection (dpi), including Nestin, GLAST, Sox2, Prominin-1, and GFAP. EGFP(+)-doublecortin (DCX) cells with a migratory morphology were also detected and their abundance increased over a 7-day period. Furthermore, EGFP-labeled cells progressively became NeuN(+) neurons, they acquired neuronal morphologies, and they became immunoreactive for OB neuron subtype markers, the most abundant representing calretinin expressing interneurons. OB-NSCs also generated glial cells, suggesting they could be multipotent in vivo. Significantly, the newly generated neurons established and received synaptic contacts, and they expressed presynaptic proteins and the transcription factor pCREB. By contrast, when the retroviral particles were injected into the subventricular zone (SVZ), nearly all (98%) EGFP(+)-cells were postmitotic when they reached the OB core, implying that the vast majority of proliferating cells present in the OB are not derived from the SVZ. Furthermore, we detected slowly dividing label-retaining cells in this region that could correspond to the population of resident NSCs. This is the first time NSCs located in the adult OB core have been shown to generate neurons that incorporate into OB circuits in vivo.

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