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p21 loss compromises the relative quiescence of forebrain stem cell proliferation leading to exhaustion of their proliferation capacity
Tod E. Kippin, David J. Martens, Derek van der Kooy
Genes & Development · 2005 · ▲ 446 citations
Abstract
Adult stem cells in various tissues are relatively quiescent. The cell cycle inhibitor p21cip1/waf1 (p21) has been shown to be important for maintaining hematopoietic stem cell quiescence and self-renewal. We examined the role of p21 in the regulation of adult mammalian forebrain neural stem cells (NSCs). We found that p21-/- mice between post-natal age 60-240 d have more NSCs than wild-type (+/+) controls due to higher proliferation rates of p21-/- NSCs. Thereafter, NSCs in p21-/- mice decline and are reduced in number at 16 mo relative to p21+/+ mice. Similarly, both p21-/- and p21+/+ NSCs display self-renewal in vitro; however, p21-/- NSCs display limited in vitro self-renewal (surviving a few passages, then exhausting). Thus, p21 contributes to adult NSC relative quiescence, which we propose is necessary for the life-long maintenance of NSC self-renewal because NSCs may be limited to a finite number of divisions.
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- 10.1101/gad.1272305
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- 2026-06-07 MST
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APA
Kippin, T.E., Martens, D.J., & Kooy, D.V.D. (2005). p21 loss compromises the relative quiescence of forebrain stem cell proliferation leading to exhaustion of their proliferation capacity. <em>Genes & Development</em>. https://doi.org/10.1101/gad.1272305
Vancouver
Kippin TE, Martens DJ, Kooy DVD. p21 loss compromises the relative quiescence of forebrain stem cell proliferation leading to exhaustion of their proliferation capacity. Genes & Development. 2005. doi:10.1101/gad.1272305.
BibTeX
@article{tod2005plossc,
title = {p21 loss compromises the relative quiescence of forebrain stem cell proliferation leading to exhaustion of their proliferation capacity},
author = {Tod E. Kippin and David J. Martens and Derek van der Kooy},
journal = {Genes & Development},
year = {2005},
doi = {10.1101/gad.1272305},
}
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