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首页> 外文期刊>Neuroscience Letters: An International Multidisciplinary Journal Devoted to the Rapid Publication of Basic Research in the Brain Sciences >Combined use of bFGF/EGF and all-trans-retinoic acid cooperatively promotes neuronal differentiation and neurite outgrowth in neural stem cells
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Combined use of bFGF/EGF and all-trans-retinoic acid cooperatively promotes neuronal differentiation and neurite outgrowth in neural stem cells

机译:联合使用BFGF / EGF和全转甲酸配合使用神经干细胞中的神经元分化和神经突生来

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摘要

Neural stem cells (NSCs) as sources of new neurons in brain injuries or diseases are required to not only elicit neurons for neuronal repair, but also to enhance neurite outgrowth for neuronal network reestablishment. Various trophic or chemotropic factors have been shown to cooperatively improve NSC neurogenesis. However, effects of combined treatment of all-trans-retinoic acid (RA) with GF (Basic fibroblast growth factor and epidermal growth factor, bFGF/EGF) on neurogenesis of NSCs are poorly understood. To address this question, NSCs were isolated from the forebrains of embryonic mice, and treated with GF and RA either alone or in combination for differentiation in vitro. Neurons and astrocytes differentiated from NSCs were stained for MAP2 and GFAP separately by immunofluorescence. The results indicated that GF displayed superior efficacy in promoting neuronal differentiation, and RA showed better efficacy in advancing neurite outgrowth by increasing both neurite length and number. In addition, higher differentiation efficiency of neurons to astrocytes in RA or GF, or both acted at the early stage. However, more importantly, compared with RA alone, GF and RA in combination enhanced neuronal differentiation. Moreover, the combined use of GF and RA increased the length and number of neurites compared with GF, as well as the relative expression level of Smurf1. In addition, astrocytes induced by GF, RA, or both exhibited a radial glia-like morphology with long processes differing from serum effects, which might in part attribute to the total numbers of neurons. These findings for the first time unveil the roles of combined use of GF and RA on the neurogenesis of NSCs, suggesting that the use of this combination could be a comprehensive strategy for the functional repair of the nervous system through promoting neuronal differentiation, and advancing neurite outgrowth.
机译:神经干细胞(NSCs)作为脑损伤或疾病的新神经元的来源,不仅需要引发神经元修复的神经元,而且还需要增强神经元网络重建的神经突遗传。已显示各种营养或趋化因子来协同改善NSC神经发生。然而,与NSCs的神经发生的GF(碱性成纤维细胞生长因子和表皮生长因子,BFGF / EGF)的组合治疗与NSCs神经发生的影响很差。为了解决这个问题,从胚胎小鼠的前脑中分离NSC,并用GF和Ra单独处理,或者组合于体外分化。通过免疫荧光分别为MAP2和GFAP染色从NSCs分化的神经元和星形胶质细胞。结果表明,GF在促进神经元分化方面显示出优异的功效,并且RA通过增加神经突长度和数量来推进神经沸石产物的更好疗效。此外,神经元对ra或gf中的星形胶质细胞的更高分化效率,或在早期作用。然而,更重要的是,与单独的RA相比,GF和RA组合中的增强神经元分化。此外,与GF相比,GF和Ra的组合使用增加了神经疾病的长度和数量,以及Smurf1的相对表达水平。此外,GF,Ra或两者诱导的星形胶质细胞表现出径向胶胶状形态,与血清效应不同的长过程,这可能与神经元的总数归因于神经元的总数。这些发现首次揭示了GF和Ra在NSC的神经发生中的组合使用的作用,表明这种组合的使用可以通过促进神经元分化和推进神经态来成为神经系统功能修复的综合策略过度。

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