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Effects of microtubule-associated protein tau expression on neural stem cell migration after spinal cord injury

机译:脊髓损伤后微管相关蛋白tau表达对神经干细胞迁移的影响

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Our preliminary proteomics analysis suggested that expression of microtubule-associated protein tau is elevated in the spinal cord after injury. Therefore, the first aim of the present study was to examine tau expression in the injured spinal cord. The second aim was to determine whether tau can regulate neural stem cell migration, a critical factor in the successful treatment of spinal cord injury. We established rat models of spinal cord injury and injected them with mouse hippocampal neural stem cells through the tail vein. We used immunohistochemistry to show that the expression of tau protein and the number of migrated neural stem cells were markedly increased in the injured spinal cord. Furthermore, using a Transwell assay, we showed that neural stem cell migration was not affected by an elevated tau concentration in the outer chamber, but it was decreased by changes in intracellular tau phosphorylation state. These results demonstrate that neural stem cells have targeted migration capability at the site of injury, and that although tau is not a chemokine for targeted migration of neural stem cells, intracellular tau phosphorylation/dephosphorylation can inhibit cell migration.
机译:我们的初步蛋白质组学分析表明,损伤后脊髓中微管相关蛋白tau的表达升高。因此,本研究的首要目的是检查受损脊髓中的tau表达。第二个目的是确定tau是否能调节神经干细胞迁移,这是成功治疗脊髓损伤的关键因素。我们建立了脊髓损伤的大鼠模型,并通过尾静脉向它们注射了小鼠海马神经干细胞。我们使用免疫组织化学显示,在受损的脊髓中,tau蛋白的表达和迁移的神经干细胞的数量明显增加。此外,使用Transwell测定法,我们发现神经干细胞迁移不受外室中tau浓度升高的影响,但会因细胞内tau磷酸化状态的改变而减少。这些结果表明神经干细胞在损伤部位具有靶向迁移能力,并且尽管tau不是神经干细胞靶向迁移的趋化因子,但是细胞内tau磷酸化/去磷酸化可以抑制细胞迁移。

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