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通过NeuroD1介导的星形胶质细胞向神经元转化实现脊髓损伤后功能性神经元的再生

Regeneration of Functional Neurons After Spinal Cord Injury via NeuroD1-Mediated Astrocyte-to-Neuron Conversion.

作者信息

Puls Brendan, Ding Yan, Zhang Fengyu, Pan Mengjie, Lei Zhuofan, Pei Zifei, Jiang Mei, Bai Yuting, Forsyth Cody, Metzger Morgan, Rana Tanvi, Zhang Lei, Ding Xiaoyun, Keefe Matthew, Cai Alice, Redilla Austin, Lai Michael, He Kevin, Li Hedong, Chen Gong

机构信息

Department of Biology, Huck Institutes of Life Sciences, The Pennsylvania State University, University Park, PA, United States.

Department of Neuroscience & Regenerative Medicine, Medical College of Georgia at Augusta University, Augusta, GA, United States.

出版信息

Front Cell Dev Biol. 2020 Dec 16;8:591883. doi: 10.3389/fcell.2020.591883. eCollection 2020.

Abstract

Spinal cord injury (SCI) often leads to impaired motor and sensory functions, partially because the injury-induced neuronal loss cannot be easily replenished through endogenous mechanisms. neuronal reprogramming has emerged as a novel technology to regenerate neurons from endogenous glial cells by forced expression of neurogenic transcription factors. We have previously demonstrated successful astrocyte-to-neuron conversion in mouse brains with injury or Alzheimer's disease by overexpressing a single neural transcription factor NeuroD1. Here we demonstrate regeneration of spinal cord neurons from reactive astrocytes after SCI through AAV NeuroD1-based gene therapy. We find that NeuroD1 converts reactive astrocytes into neurons in the dorsal horn of stab-injured spinal cord with high efficiency (~95%). Interestingly, NeuroD1-converted neurons in the dorsal horn mostly acquire glutamatergic neuronal subtype, expressing spinal cord-specific markers such as Tlx3 but not brain-specific markers such as Tbr1, suggesting that the astrocytic lineage and local microenvironment affect the cell fate after conversion. Electrophysiological recordings show that the NeuroD1-converted neurons can functionally mature and integrate into local spinal cord circuitry by displaying repetitive action potentials and spontaneous synaptic responses. We further show that NeuroD1-mediated neuronal conversion can occur in the contusive SCI model with a long delay after injury, allowing future studies to further evaluate this reprogramming technology for functional recovery after SCI. In conclusion, this study may suggest a paradigm shift from classical axonal regeneration to neuronal regeneration for spinal cord repair, using astrocyte-to-neuron conversion technology to regenerate functional new neurons in the gray matter.

摘要

脊髓损伤(SCI)常常导致运动和感觉功能受损,部分原因是损伤诱导的神经元丢失难以通过内源性机制轻易补充。神经元重编程已成为一种新技术,可通过强制表达神经源性转录因子,从内源性神经胶质细胞再生神经元。我们之前已经证明,通过过表达单一神经转录因子NeuroD1,在受伤或患有阿尔茨海默病的小鼠大脑中,成功实现了星形胶质细胞向神经元的转化。在此,我们通过基于腺相关病毒(AAV)NeuroD1的基因疗法,证明了脊髓损伤后反应性星形胶质细胞可再生脊髓神经元。我们发现,NeuroD1能高效地(约95%)将刺伤脊髓背角中的反应性星形胶质细胞转化为神经元。有趣的是,背角中经NeuroD1转化的神经元大多获得谷氨酸能神经元亚型,表达脊髓特异性标志物如Tlx3,但不表达脑特异性标志物如Tbr1,这表明星形胶质细胞谱系和局部微环境会影响转化后的细胞命运。电生理记录显示,经NeuroD1转化的神经元能够在功能上成熟,并通过显示重复性动作电位和自发突触反应,整合到局部脊髓回路中。我们进一步表明,NeuroD1介导的神经元转化可在挫伤性脊髓损伤模型中在损伤后很长时间发生,这使得未来的研究能够进一步评估这种重编程技术对脊髓损伤后功能恢复的作用。总之,本研究可能意味着脊髓修复从经典的轴突再生向神经元再生的范式转变,利用星形胶质细胞向神经元的转化技术在灰质中再生功能性新神经元。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3c76/7793709/037860fc5d58/fcell-08-591883-g0001.jpg

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