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内源性成年神经祖细胞对小鼠急性脊髓损伤的早期反应

Early response of endogenous adult neural progenitor cells to acute spinal cord injury in mice.

作者信息

Ke Yan, Chi Liying, Xu Renshi, Luo Chun, Gozal David, Liu Rugao

机构信息

Department of Anatomy and Cell Biology, University of North Dakota School of Medicine, Grand Forks, North Dakota 58202, USA.

出版信息

Stem Cells. 2006 Apr;24(4):1011-9. doi: 10.1634/stemcells.2005-0249. Epub 2005 Dec 8.

Abstract

Adult neural progenitor cells (NPCs) are an attractive source for functional replacement in neurodegenerative diseases and traumatic injury to the central nervous system (CNS). It has been shown that transplantation of neural stem cells or NPCs into the lesioned region partially restores CNS function. However, the capacity of endogenous NPCs in replacement of neuronal cell loss and functional recovery of spinal cord injury (SCI) is apparently poor. Furthermore, the temporal and spatial response of endogenous adult NPCs to SCI remains largely undefined. To this end, we have analyzed the early organization, distribution, and potential function of NPCs in response to SCI, using nestin enhancer (promoter) controlled LacZ reporter transgenic mice. We showed that there was an increase of NPC proliferation, migration, and neurogenesis in adult spinal cord after traumatic compression SCI. The proliferation of NPCs detected by 5-bromodeoxyuridine incorporation and LacZ staining was restricted to the ependymal zone (EZ) of the central canal. During acute SCI, NPCs in the EZ of the central canal migrated vigorously toward the dorsal direction, where the compression lesion is generated. The optimal NPC migration occurred in the adjacent region close to the epicenter. More significantly, there was an increased de novo neurogenesis from NPCs 24 hours after SCI. The enhanced proliferation, migration, and neurogenesis of (from) endogenous NPCs in the adult spinal cord in response to SCI suggest a potential role for NPCs in attempting to restore SCI-mediated neuronal dysfunction.

摘要

成年神经祖细胞(NPCs)是神经退行性疾病和中枢神经系统(CNS)创伤性损伤中进行功能替代的一个有吸引力的细胞来源。研究表明,将神经干细胞或NPCs移植到损伤区域可部分恢复中枢神经系统功能。然而,内源性NPCs在替代脊髓损伤(SCI)后神经元细胞丢失和功能恢复方面的能力明显较差。此外,内源性成年NPCs对SCI的时空反应在很大程度上仍不明确。为此,我们利用巢蛋白增强子(启动子)控制的LacZ报告基因转基因小鼠,分析了NPCs对SCI的早期组织、分布及潜在功能。我们发现,创伤性压迫性SCI后成年脊髓中NPCs的增殖、迁移和神经发生增加。通过5-溴脱氧尿苷掺入和LacZ染色检测到的NPCs增殖局限于中央管的室管膜区(EZ)。在急性SCI期间,中央管EZ中的NPCs强烈地向背侧方向迁移,即产生压迫性损伤的部位。最佳的NPC迁移发生在靠近震中的相邻区域。更显著的是,SCI后24小时NPCs产生的新生神经发生增加。成年脊髓中内源性NPCs对SCI的增殖、迁移和神经发生增强表明,NPCs在试图恢复SCI介导的神经元功能障碍方面具有潜在作用。

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