星形胶质细胞作为髓磷脂和Ranvier淋巴结参与抑郁和应激相关疾病病理生理的背景。

José Javier Miguel-Hidalgo
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引用次数: 3

摘要

星形胶质细胞虽然具有支持灰质和白质神经元功能的神经胶质细胞的一些共同特征,但在特定的神经环境中,星形胶质细胞参与并调整其形态和神经化学,参与大量不同的调节任务。在白质中,大部分从星形胶质细胞细胞体分支出来的突与少突胶质细胞及其形成的髓鞘建立了接触,而许多星形胶质细胞分支的尖端与Ranvier结密切相关。髓磷脂的稳定性在很大程度上依赖于星形胶质细胞与少突胶质细胞之间的通讯,而在Ranvier节点再生的动作电位的完整性则主要依赖于星形胶质细胞贡献的细胞外基质成分。几条线索的证据开始表明,在情感障碍的人类受试者和慢性应激的动物模型中,髓磷脂成分、白质星形胶质细胞和兰维耶淋巴结发生了重大变化,这些变化与这些疾病的连通性改变直接相关。其中一些变化涉及支持星形胶质细胞与少突胶质细胞间隙连接的连接蛋白的表达、Ranvier淋巴结周围星形胶质细胞产生的细胞外基质成分、特定类型的星形胶质细胞谷氨酸转运蛋白以及参与髓磷脂发育和可塑性的星形胶质细胞分泌的神经营养因子。未来的研究应该进一步研究白质星形胶质细胞变化的机制,它们对情感性疾病病理连接的假定贡献,以及利用这些知识设计精神疾病新疗法的可能性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Astrocytes as Context for the Involvement of Myelin and Nodes of Ranvier in the Pathophysiology of Depression and Stress-Related Disorders.

Astrocytes, despite some shared features as glial cells supporting neuronal function in gray and white matter, participate and adapt their morphology and neurochemistry in a plethora of distinct regulatory tasks in specific neural environments. In the white matter, a large proportion of the processes branching from the astrocytes' cell bodies establish contacts with oligodendrocytes and the myelin they form, while the tips of many astrocyte branches closely associate with nodes of Ranvier. Stability of myelin has been shown to greatly depend on astrocyte-to-oligodendrocyte communication, while the integrity of action potentials that regenerate at nodes of Ranvier has been shown to depend on extracellular matrix components heavily contributed by astrocytes. Several lines of evidence are starting to show that in human subjects with affective disorders and in animal models of chronic stress there are significant changes in myelin components, white matter astrocytes and nodes of Ranvier that have direct relevance to connectivity alterations in those disorders. Some of these changes involve the expression of connexins supporting astrocyte-to-oligodendrocyte gap junctions, extracellular matrix components produced by astrocytes around nodes of Ranvier, specific types of astrocyte glutamate transporters, and neurotrophic factors secreted by astrocytes that are involved in the development and plasticity of myelin. Future studies should further examine the mechanisms responsible for those changes in white matter astrocytes, their putative contribution to pathological connectivity in affective disorders, and the possibility of leveraging that knowledge to design new therapies for psychiatric disorders.

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