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尽管老年大脑中的神经干细胞和祖细胞数量较少,但它们仍保留着增殖和分化为功能性神经元的潜力。

Neural stem and progenitor cells retain their potential for proliferation and differentiation into functional neurons despite lower number in aged brain.

作者信息

Ahlenius Henrik, Visan Violeta, Kokaia Merab, Lindvall Olle, Kokaia Zaal

机构信息

Laboratory of Neural Stem Cell Biology, Experimental Epilepsy Group, Section of Restorative Neurology, Wallenberg Neuroscience Center, University Hospital, SE-221 84 Lund, Sweden.

出版信息

J Neurosci. 2009 Apr 8;29(14):4408-19. doi: 10.1523/JNEUROSCI.6003-08.2009.

Abstract

Neurogenesis in the subventricular zone (SVZ), which gives rise to new neurons in the olfactory bulb, continues throughout life but declines with increasing age. Little is known about how aging affects the intrinsic properties of the neural stem and progenitor cells (NSCs) in SVZ and the functional characteristics of their neuronal progeny. Here, we have compared the properties of NSCs isolated from embryonic lateral ganglionic eminence and adult and aged SVZ in mice using in vivo and in vitro systems, analyzed their gene expression profile, and studied their electrophysiological characteristics before and after differentiation into neurons. We show a loss of NSCs in SVZ from aged mice accompanied by reduced expression of genes for NSC markers, developmentally important transcription factors, and neurogenic factors. However, when isolated in vitro, the NSCs from SVZ of aged animals have capacity for proliferation and multilineage differentiation, including production of functional neurons, similar to that of NSCs in adult mice, albeit with lower efficacy. These properties are of major importance when considering therapeutic applications of neuronal replacement from endogenous NSCs in the injured, aged brain.

摘要

脑室下区(SVZ)的神经发生可产生嗅球中的新神经元,这种神经发生在整个生命过程中持续存在,但会随着年龄的增长而减少。关于衰老如何影响SVZ中神经干细胞和祖细胞(NSCs)的内在特性以及它们神经元后代的功能特征,我们知之甚少。在这里,我们使用体内和体外系统比较了从小鼠胚胎侧神经节隆起、成年和老年SVZ中分离出的NSCs的特性,分析了它们的基因表达谱,并研究了它们分化为神经元前后的电生理特征。我们发现老年小鼠SVZ中的NSCs数量减少,同时NSC标志物、发育重要转录因子和神经发生因子的基因表达降低。然而,当在体外分离时,老年动物SVZ中的NSCs具有增殖和多谱系分化的能力,包括产生功能性神经元,这与成年小鼠中的NSCs相似,尽管效率较低。在考虑从内源性NSCs进行神经元替代治疗受损的老年大脑时,这些特性至关重要。

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