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首页> 外文期刊>Cell transplantation >Bone marrow contributes simultaneously to different neural types in the central nervous system through different mechanisms of plasticity.
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Bone marrow contributes simultaneously to different neural types in the central nervous system through different mechanisms of plasticity.

机译:骨髓通过不同的可塑性机制同时为中枢神经系统的不同神经类型做出贡献。

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摘要

Many studies have reported the contribution of bone marrow-derived cells (BMDC) to the CNS, raising the possibility of using them as a new source to repair damaged brain tissue or restore neuronal function. This process has mainly been investigated in the cerebellum, in which a degenerative microenvironment has been suggested to be responsible for its modulation. The present study further analyzes the contribution of BMDC to different neural types in other adult brain areas, under both physiological and neurodegenerative conditions, together with the mechanisms of plasticity involved. We grafted genetically marked green fluorescent protein/Cre bone marrow in irradiated recipients: a) the PCD (Purkinje Cell Degeneration) mutant mice, suffering a degeneration of specific neuronal populations at different ages, and b) their corresponding healthy controls. These mice carried the conditional lacZ reporter gene to allow the identification of cell fusion events. Our results demonstrate that BMDC mainly generate microglial cells, although to a lesser extent a clear formation of neuronal types also exists. This neuronal recruitment was not increased by the neurodegenerative processes occurring in PCD mice, where BMDC did not contribute to rescuing the degenerated neuronal populations either. However, an increase in the number of bone marrow-derived microglia was found along the life span in both experimental groups. Six weeks after transplantation more bone marrow-derived microglial cells were observed in the olfactory bulb of the PCD mice compared to the control animals, where the degeneration of mitral cells was in process. In contrast, this difference was not observed in the cerebellum, where Purkinje cell degeneration had been completed. These findings demonstrated that the degree of neurodegenerative environment can foster the recruitment of neural elements derived from bone marrow, but also provide the first evidence that BMDC can contribute simultaneously to different encephalic areas through different mechanisms of plasticity: cell fusion for Purkinje cells and differentiation for olfactory bulb interneurons.
机译:许多研究报道了骨髓源性细胞(BMDC)对中枢神经系统的贡献,从而增加了将其用作修复受损脑组织或恢复神经元功能的新来源的可能性。该过程主要在小脑中进行了研究,在该小脑中,退化的微环境被认为是其调控的原因。本研究进一步分析了BMDC对其他成年大脑区域在生理和神经变性条件下不同神经类型的贡献,以及所涉及的可塑性机制。我们在受辐照的受体中移植了遗传标记的绿色荧光蛋白/ Cre骨髓:a)PCD(浦肯野细胞变性)突变小鼠,在不同年龄遭受特定神经元群体的变性,b)其相应的健康对照。这些小鼠携带条件lacZ报告基因,以鉴定细胞融合事件。我们的结果表明,BMDC主要产生小胶质细胞,尽管在较小程度上也存在明显的神经元类型形成。在PCD小鼠中发生的神经变性过程并未增加这种神经元募集,其中BMDC也不有助于挽救退化的神经元种群。然而,在两个实验组中,发现整个生命过程中骨髓来源的小胶质细胞数量增加。移植后六周,与对照组动物相比,在PCD小鼠的嗅球中观察到更多的骨髓来源的小胶质细胞,而在对照组动物中二尖瓣细胞正在退化。相反,在完成浦肯野细胞变性的小脑中没有观察到这种差异。这些发现表明,神经退行性环境的程度可以促进骨髓来源的神经元的募集,但也提供了第一个证据,表明BMDC可以通过不同的可塑性机制同时对不同的脑区域做出贡献:Purkinje细胞的细胞融合和嗅球interneurons。

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