p107 regulates neural precursor cells in the mammalian brain |
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Authors: | Vanderluit Jacqueline L Ferguson Kerry L Nikoletopoulou Vassiliki Parker Maura Ruzhynsky Vladimir Alexson Tania McNamara Stephen M Park David S Rudnicki Michael Slack Ruth S |
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Affiliation: | Neuroscience Research Group, Ottawa Health Research Institute, Ottawa, Ontario, Canada. |
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Abstract: | Here we show a novel function for Retinoblastoma family member, p107 in controlling stem cell expansion in the mammalian brain. Adult p107-null mice had elevated numbers of proliferating progenitor cells in their lateral ventricles. In vitro neurosphere assays revealed striking increases in the number of neurosphere forming cells from p107(-/-) brains that exhibited enhanced capacity for self-renewal. An expanded stem cell population in p107-deficient mice was shown in vivo by (a) increased numbers of slowly cycling cells in the lateral ventricles; and (b) accelerated rates of neural precursor repopulation after progenitor ablation. Notch1 was up-regulated in p107(-/-) neurospheres in vitro and brains in vivo. Chromatin immunoprecipitation and p107 overexpression suggest that p107 may modulate the Notch1 pathway. These results demonstrate a novel function for p107 that is distinct from Rb, which is to negatively regulate the number of neural stem cells in the developing and adult brain. |
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Keywords: | neural stem cells self-renewing division regeneration |
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