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体外培养的海马放射状胶质细胞中的基质细胞衍生因子-1α调节神经祖细胞的迁移。

Stromal derived factor-1α in hippocampus radial glial cells in vitro regulates the migration of neural progenitor cells.

作者信息

Ding Hui, Jin Guo-Hua, Zou Lin-Qing, Zhang Xiao-Qing, Li Hao-Ming, Tao Xue-Lei, Zhang Xin-Hua, Qin Jian-Bing, Tian Mei-Ling

机构信息

Department of Anatomy and Neurobiology, The Jiangsu Key Laboratory of Neuroregeneration, Nantong University, Co-innovation Center of Neuroregeneration, Nantong, Jiangsu Province, 226001, People's Republic of China.

出版信息

Cell Biol Int. 2015 Jun;39(6):750-8. doi: 10.1002/cbin.10442. Epub 2015 Feb 2.

Abstract

Stromal derived factor-1α (SDF-1α), a critical chemokine that promotes cell homing to target tissues, was presumed to be involved in the traumatic brain injury cortex. In this study, we determined the expression of SDF-1α in the hippocampus after transection of the fimbria fornix (FF). Realtime PCR and ELISA showed that mRNA transcription and SDF-1α proteins increased significantly after FF transection. In vitro, the expression of SDF-1α in radial glial cells (RGCs) incubated with deafferented hippocampus extracts was observed to be greater than in those incubated with normal hippocampus extracts. The co-culture of neural progenitor cells (NPCs) and RGCs indicated that the extracts of deafferented hippocampus induced more NPCs migrating toward RGCs than the normal extracts. Suppression or overexpression of SDF-1α in RGCs markedly either decreased or increased, respectively, the migration of NPCs. These results suggest that after FF transection, SDF-1α in the deafferented hippocampus was upregulated and might play an important role in RGC induction of NPC migration; therefore, SDF-1α is a target for additional research for determining new therapy for brain injuries.

摘要

基质衍生因子-1α(SDF-1α)是一种促进细胞归巢至靶组织的关键趋化因子,被推测与创伤性脑损伤皮质有关。在本研究中,我们测定了穹窿海马伞(FF)横断后海马中SDF-1α的表达。实时定量PCR和酶联免疫吸附测定显示,FF横断后mRNA转录和SDF-1α蛋白显著增加。在体外,观察到与去传入海马提取物孵育的放射状胶质细胞(RGCs)中SDF-1α的表达高于与正常海马提取物孵育的细胞。神经祖细胞(NPCs)与RGCs的共培养表明,去传入海马提取物比正常提取物诱导更多的NPCs向RGCs迁移。RGCs中SDF-1α的抑制或过表达分别显著降低或增加了NPCs的迁移。这些结果表明,FF横断后,去传入海马中的SDF-1α上调,可能在RGCs诱导NPCs迁移中起重要作用;因此,SDF-1α是确定脑损伤新疗法的进一步研究靶点。

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