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成体海马神经发生中的中间祖细胞:Tbr2表达与神经元输出的协同调控。

Intermediate progenitors in adult hippocampal neurogenesis: Tbr2 expression and coordinate regulation of neuronal output.

作者信息

Hodge Rebecca D, Kowalczyk Thomas D, Wolf Susanne A, Encinas Juan M, Rippey Caitlin, Enikolopov Grigori, Kempermann Gerd, Hevner Robert F

机构信息

Department of Neurological Surgery, University of Washington School of Medicine, Seattle, Washington 98101-1304, USA.

出版信息

J Neurosci. 2008 Apr 2;28(14):3707-17. doi: 10.1523/JNEUROSCI.4280-07.2008.

Abstract

Neurogenesis in the adult hippocampus is a highly regulated process that originates from multipotent progenitors in the subgranular zone (SGZ). Currently, little is known about molecular mechanisms that regulate proliferation and differentiation in the SGZ. To study the role of transcription factors (TFs), we focused on Tbr2 (T-box brain gene 2), which has been implicated previously in developmental glutamatergic neurogenesis. In adult mouse hippocampus, Tbr2 protein and Tbr2-GFP (green fluorescent protein) transgene expression were specifically localized to intermediate-stage progenitor cells (IPCs), a type of transit amplifying cells. The Tbr2+ IPCs were highly responsive to neurogenic stimuli, more than doubling after voluntary wheel running. Notably, the Tbr2+ IPCs formed cellular clusters, the average size of which (Tbr2+ cells per cluster) likewise more than doubled in runners. Conversely, Tbr2+ IPCs were selectively depleted by antimitotic drugs, known to suppress neurogenesis. After cessation of antimitotic treatment, recovery of neurogenesis was paralleled by recovery of Tbr2+ IPCs, including a transient rebound above baseline numbers. Finally, Tbr2 was examined in the context of additional TFs that, together, define a TF cascade in embryonic neocortical neurogenesis (Pax6 --> Ngn2 --> Tbr2 --> NeuroD --> Tbr1). Remarkably, the same TF cascade was found to be linked to stages of neuronal lineage progression in adult SGZ. These results suggest that Tbr2+ IPCs play a major role in the regulation of adult hippocampal neurogenesis, and that a similar transcriptional program controls neurogenesis in adult SGZ as in embryonic cerebral cortex.

摘要

成体海马体中的神经发生是一个受到高度调控的过程,起源于颗粒下区(SGZ)的多能祖细胞。目前,对于调控SGZ中细胞增殖和分化的分子机制知之甚少。为了研究转录因子(TFs)的作用,我们聚焦于Tbr2(T-box脑基因2),它先前已被证明与发育过程中的谷氨酸能神经发生有关。在成年小鼠海马体中,Tbr2蛋白和Tbr2-绿色荧光蛋白(GFP)转基因表达特异性定位于中间阶段祖细胞(IPCs),这是一种过渡增殖细胞。Tbr2+ IPCs对神经发生刺激高度敏感,在自愿转轮运动后数量增加一倍以上。值得注意的是,Tbr2+ IPCs形成细胞簇,其平均大小(每个簇中的Tbr2+细胞数)在跑步小鼠中同样增加了一倍以上。相反,Tbr2+ IPCs被已知可抑制神经发生的抗有丝分裂药物选择性消耗。抗有丝分裂治疗停止后,神经发生的恢复与Tbr2+ IPCs的恢复平行,包括短暂超过基线数量的反弹。最后,在其他转录因子的背景下研究了Tbr2,这些转录因子共同定义了胚胎新皮质神经发生中的一个转录因子级联(Pax6 --> Ngn2 --> Tbr2 --> NeuroD --> Tbr1)。值得注意的是,发现相同的转录因子级联与成年SGZ中神经元谱系进展的阶段相关。这些结果表明,Tbr2+ IPCs在成年海马体神经发生的调控中起主要作用,并且类似的转录程序控制成年SGZ中的神经发生,就像在胚胎大脑皮质中一样。

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