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暴露于ROCK抑制剂法舒地尔可促进神经干细胞在体外发生神经胶质生成。

Exposure to the ROCK inhibitor fasudil promotes gliogenesis of neural stem cells in vitro.

作者信息

Nizamudeen Zubair Ahmed, Chakrabarti Lisa, Sottile Virginie

机构信息

Wolfson STEM Centre, School of Medicine, University of Nottingham, UK.

School of Veterinary Science, University of Nottingham, UK.

出版信息

Stem Cell Res. 2018 Apr;28:75-86. doi: 10.1016/j.scr.2018.02.001. Epub 2018 Feb 6.

Abstract

Fasudil is a clinically approved Rho-associated protein kinase (ROCK) inhibitor that has been used widely to treat cerebral consequences of subarachnoid hemorrhage. It is known to have a positive effect on animal models of neurological disorders including Parkinson's disease and stroke. However, its cellular effect on progenitor populations and differentiation is not clearly understood. While recent studies suggest that fasudil promotes the mobilization of neural stem cells (NSCs) from the subventricular zone in vivo and promotes the differentiation of the C17.2 cerebellar neuroprogenitor line in vitro, it is unclear whether fasudil is involved in the differentiation of primary NSCs. Here, we tested the effect of fasudil on mouse NSCs in vitro, and observed increased gliogenesis in NSCs derived from lateral ventricles. Upon treatment, fasudil promoted characteristics of neurogenesis including phenotypic changes in neural outgrowth and interkinetic nuclear-like movements as an immediate response, while Sox2 expression was maintained and GFAP expression increased. Moreover, the gliogenic response to fasudil medium was observed in both early postnatal and adult NSC cultures. Taken together, our results show that fasudil promotes the differentiation of NSCs into astroglial lineage, suggesting that it could be used to develop novel vitro gliogenesis models and regulate differentiation for neural repair.

摘要

法舒地尔是一种临床批准的Rho相关蛋白激酶(ROCK)抑制剂,已被广泛用于治疗蛛网膜下腔出血的脑部后果。已知它对包括帕金森病和中风在内的神经疾病动物模型有积极作用。然而,其对祖细胞群体和分化的细胞效应尚不清楚。虽然最近的研究表明,法舒地尔在体内促进神经干细胞(NSCs)从脑室下区的动员,并在体外促进C17.2小脑神经祖细胞系的分化,但尚不清楚法舒地尔是否参与原代NSCs的分化。在这里,我们在体外测试了法舒地尔对小鼠NSCs的作用,并观察到源自侧脑室的NSCs中胶质细胞生成增加。处理后,法舒地尔立即促进神经发生的特征,包括神经突起的表型变化和核间运动,同时维持Sox2表达并增加GFAP表达。此外,在出生后早期和成年NSC培养物中均观察到对法舒地尔培养基的胶质细胞生成反应。综上所述,我们的结果表明,法舒地尔促进NSCs向星形胶质细胞谱系的分化,这表明它可用于开发新的体外胶质细胞生成模型并调节神经修复的分化。

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