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FoxO3 regulates neural stem cell homeostasis.

机译:FoxO3调节神经干细胞稳态。

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In the nervous system, neural stem cells (NSCs) are necessary for the generation of new neurons and for cognitive function. Here we show that FoxO3, a member of a transcription factor family known to extend lifespan in invertebrates, regulates the NSC pool. We find that adult FoxO3(-/-) mice have fewer NSCs in vivo than wild-type counterparts. NSCs isolated from adult FoxO3(-/-) mice have decreased self-renewal and an impaired ability to generate different neural lineages. Identification of the FoxO3-dependent gene expression profile in NSCs suggests that FoxO3 regulates the NSC pool by inducing a program of genes that preserves quiescence, prevents premature differentiation, and controls oxygen metabolism. The ability of FoxO3 to prevent the premature depletion of NSCs might have important implications for counteracting brain aging in long-lived species.
机译:在神经系统中,神经干细胞(NSC)是产生新神经元和认知功能所必需的。在这里,我们显示FoxO3是已知可延长无脊椎动物寿命的转录因子家族的成员,它调节NSC库。我们发现,成年FoxO3(-/-)小鼠体内的NSC比野生型小鼠少。从成年FoxO3(-/-)小鼠中分离出的NSC自我更新能力下降,并且产生不同神经谱系的能力受损。对NSC中FoxO3依赖性基因表达谱的鉴定表明,FoxO3通过诱导可保持静止,防止过早分化并控制氧代谢的基因程序来调节NSC库。 FoxO3防止NSCs提前枯竭的能力可能对抵抗长寿物种的大脑衰老具有重要意义。

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