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间质干细胞增强共培养海马神经元中的 GABA 能传递。

Mesenchymal stem cells enhance GABAergic transmission in co-cultured hippocampal neurons.

机构信息

Department of Experimental Medicine, University of Milano-Bicocca, Via Cadore 48, 20900 Monza, Italy.

出版信息

Mol Cell Neurosci. 2012 Apr;49(4):395-405. doi: 10.1016/j.mcn.2012.02.004. Epub 2012 Feb 23.

Abstract

Bone marrow-derived mesenchymal stem cells (MSCs) are multipotent stem cells endowed with neurotrophic potential combined with immunological properties, making them a promising therapeutic tool for neurodegenerative disorders. However, the mechanisms through which MSCs promote the neurological recovery following injury or inflammation are still largely unknown, although cell replacement and paracrine mechanisms have been hypothesized. In order to find out what are the mechanisms of the trophic action of MSCs, as compared to glial cells, on CNS neurons, we set up a co-culture system where rat MSCs (or cortical astrocytes) were used as a feeding layer for hippocampal neurons without any direct contact between the two cell types. The analysis of hippocampal synaptogenesis, synaptic vesicle recycling and electrical activity show that MSCs were capable to support morphological and functional neuronal differentiation. The proliferation of hippocampal glial cells induced by the release of bioactive substance(s) from MSCs was necessary for neuronal survival. Furthermore, MSCs selectively increased hippocampal GABAergic pre-synapses. This effect was paralleled with a higher expression of the potassium/chloride KCC2 co-transporter and increased frequency and amplitude of mIPSCs and sIPSCs. The enhancement of GABA synapses was impaired by the treatment with K252a, a Trk/neurotrophin receptor blocker, and by TrkB receptor bodies hence suggesting the involvement of BDNF as a mediator of such effects. The results obtained here indicate that MSC-secreted factors induce glial-dependent neuronal survival and trigger an augmented GABAergic transmission in hippocampal cultures, highlighting a new effect by which MSCs could promote CNS repair. Our results suggest that MSCs may be useful in those neurological disorders characterized by an impairment of excitation versus inhibition balance.

摘要

骨髓间充质干细胞(MSCs)是具有神经营养潜力的多能干细胞,结合免疫特性,使其成为神经退行性疾病有前途的治疗工具。然而,MSCs 促进损伤或炎症后神经恢复的机制在很大程度上仍然未知,尽管已经假设了细胞替代和旁分泌机制。为了了解与神经胶质细胞相比,MSCs 对中枢神经系统神经元的营养作用的机制,我们建立了一种共培养系统,其中大鼠 MSCs(或皮质星形胶质细胞)作为海马神经元的饲养层,两种细胞类型之间没有任何直接接触。对海马突触发生、突触小泡再循环和电活动的分析表明,MSCs 能够支持形态和功能神经元分化。MSCs 释放的生物活性物质诱导海马神经胶质细胞增殖对于神经元存活是必要的。此外,MSCs 选择性增加海马 GABA 能前突触。这种效应伴随着钾/氯离子 KCC2 共转运体的更高表达以及 mIPSCs 和 sIPSCs 的频率和幅度增加。用 K252a(一种 Trk/神经营养因子受体阻滞剂)和 TrkB 受体体处理会损害 GABA 突触的增强,这表明 BDNF 作为这种效应的介质参与其中。这里获得的结果表明,MSC 分泌的因子诱导神经胶质细胞依赖性神经元存活,并在海马培养物中引发增强的 GABA 能传递,突出了 MSC 促进中枢神经系统修复的新作用。我们的结果表明,MSCs 可能对那些以兴奋与抑制平衡受损为特征的神经紊乱具有治疗作用。

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