Programmed cell death of adult-generated hippocampal neurons is mediated by the proapoptotic gene Bax
- Authors
- Sun, W; Winseck, A; Vinsant, S; Park, OH; Kim, H; Oppenheim, RW
- Issue Date
- 8-12월-2004
- Publisher
- SOC NEUROSCIENCE
- Keywords
- adult neurogenesis; Bax; cell death; mouse; proliferation; migration; differentiation
- Citation
- JOURNAL OF NEUROSCIENCE, v.24, no.49, pp.11205 - 11213
- Indexed
- SCIE
SCOPUS
- Journal Title
- JOURNAL OF NEUROSCIENCE
- Volume
- 24
- Number
- 49
- Start Page
- 11205
- End Page
- 11213
- URI
- https://scholar.korea.ac.kr/handle/2021.sw.korea/123586
- DOI
- 10.1523/JNEUROSCI.1436-04.2004
- ISSN
- 0270-6474
- Abstract
- In the dentate gyrus (DG) of the adult mouse hippocampus, a substantial number of new cells are generated daily, but only a subset of these survive and differentiate into mature neurons, whereas the majority undergo programmed cell death (PCD). However, neither the intracellular machinery required for adult stem cell-derived neuronal death nor the biological implications of the significant loss of these newly generated cells have been examined. Several markers for apoptosis failed to reveal cell death in Bax-deficient mice, and this, together with a progressive increase in neuron number in the DG of the Bax knock-out, indicates that Bax is critical for the PCD of adult-generated hippocampal neurons. Whereas the proliferation of neural progenitor cells was not altered in the Bax-knock-out, there was an accumulation of doublecortin, calretinin(+), and neuronal-specific nuclear protein(+) postmitotic neurons, suggesting that Bax-mediated PCD of adult-generated neurons takes place during an early phase of differentiation. The absence of PCD in the adult also influenced the migration and maturation of adult-generated DG neurons. These results suggest that PCD in the adult brain plays a significant role in the regulation of multiple aspects of adult neurogenesis.
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