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脑损伤和阿尔茨海默病模型中反应性神经胶质细胞在体直接重编程为功能性神经元。

In vivo direct reprogramming of reactive glial cells into functional neurons after brain injury and in an Alzheimer's disease model.

机构信息

Department of Biology, The Huck Institutes of Life Sciences, The Pennsylvania State University, University Park, PA 16802, USA.

Department of Biology, The Huck Institutes of Life Sciences, The Pennsylvania State University, University Park, PA 16802, USA.

出版信息

Cell Stem Cell. 2014 Feb 6;14(2):188-202. doi: 10.1016/j.stem.2013.12.001. Epub 2013 Dec 19.

Abstract

Loss of neurons after brain injury and in neurodegenerative disease is often accompanied by reactive gliosis and scarring, which are difficult to reverse with existing treatment approaches. Here, we show that reactive glial cells in the cortex of stab-injured or Alzheimer's disease (AD) model mice can be directly reprogrammed into functional neurons in vivo using retroviral expression of a single neural transcription factor, NeuroD1. Following expression of NeuroD1, astrocytes were reprogrammed into glutamatergic neurons, while NG2 cells were reprogrammed into glutamatergic and GABAergic neurons. Cortical slice recordings revealed both spontaneous and evoked synaptic responses in NeuroD1-converted neurons, suggesting that they integrated into local neural circuits. NeuroD1 expression was also able to reprogram cultured human cortical astrocytes into functional neurons. Our studies therefore suggest that direct reprogramming of reactive glial cells into functional neurons in vivo could provide an alternative approach for repair of injured or diseased brain.

摘要

脑损伤和神经退行性疾病后神经元的丢失通常伴随着反应性神经胶质增生和瘢痕形成,这是现有治疗方法难以逆转的。在这里,我们通过逆转录病毒表达单个神经转录因子 NeuroD1 显示,皮质中反应性神经胶质细胞可以在体内直接被重编程为功能性神经元。NeuroD1 表达后,星形胶质细胞被重编程为谷氨酸能神经元,而 NG2 细胞被重编程为谷氨酸能和 GABA 能神经元。皮层切片记录显示,NeuroD1 转化的神经元中存在自发和诱发的突触反应,表明它们整合到局部神经回路中。NeuroD1 的表达也能够将培养的人皮质星形胶质细胞重编程为功能性神经元。因此,我们的研究表明,体内将反应性神经胶质细胞直接重编程为功能性神经元可能为修复受损或患病的大脑提供了一种替代方法。

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