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胶质细胞是双相情感障碍病理生理学和治疗中的关键要素。

Glial cells as key elements in the pathophysiology and treatment of bipolar disorder.

作者信息

Keshavarz Mojtaba

机构信息

Shiraz Neuroscience Research Center,Shiraz University of Medical Sciences,Shiraz,Iran.

出版信息

Acta Neuropsychiatr. 2017 Jun;29(3):140-152. doi: 10.1017/neu.2016.56. Epub 2016 Oct 24.

Abstract

OBJECTIVE

The exact pathophysiology of bipolar disorder (BD) is not yet fully understood, and there are many questions in this area which should be answered. This review aims to discuss the roles of glial cells in the pathophysiology of BD and their contribution to the mechanism of action of mood-stabilising drugs.

METHODS

We critically reviewed the most recent advances regarding glial cell roles in the pathophysiology and treatment of BD and the neuroprotective and neurotrophic effects of these cells.

RESULTS

Postmortem studies revealed a decrease in the glial cell number or density in the specific layers of prefrontal and anterior cingulate cortex in the patients with BD, whereas there was no difference in other brain regions, such as entorhinal cortex, amygdala and hippocampus. Astrocytes and oligodendrocytes were the most important glial types that were responsible for the glial reduction, but microglia activation rather than loss may be implicated in BD. The decreased number or density of glial cells may contribute to the pathological changes observed in neurons in the patients with BD. Alteration of specific neurotrophic factors such as glial cell line-derived neurotrophic factor and S100B may be an important feature of BD. Glial cells mediate the therapeutic effects of mood-stabilising agents in the treatment of BD.

CONCLUSION

Recent studies provide important evidence on the impairment of glial cells in the pathophysiology and treatment of BD. However, future controlled studies are necessary to elucidate different aspects of glial cells contribution to BD, and the mechanism of action of mood-stabilising drugs.

摘要

目的

双相情感障碍(BD)的确切病理生理学尚未完全明了,该领域存在许多有待解答的问题。本综述旨在探讨胶质细胞在BD病理生理学中的作用及其对心境稳定剂作用机制的贡献。

方法

我们严格审查了有关胶质细胞在BD病理生理学和治疗中的作用以及这些细胞的神经保护和神经营养作用的最新进展。

结果

尸检研究显示,BD患者前额叶和前扣带回皮质特定层的胶质细胞数量或密度降低,而在内嗅皮质、杏仁核和海马体等其他脑区则无差异。星形胶质细胞和少突胶质细胞是导致胶质细胞减少的最重要胶质细胞类型,但小胶质细胞激活而非缺失可能与BD有关。胶质细胞数量或密度的降低可能导致BD患者神经元中观察到的病理变化。胶质细胞源性神经营养因子和S100B等特定神经营养因子的改变可能是BD的一个重要特征。胶质细胞介导心境稳定剂在BD治疗中的疗效。

结论

最近的研究为胶质细胞在BD病理生理学和治疗中的损伤提供了重要证据。然而,未来需要进行对照研究,以阐明胶质细胞对BD的贡献以及心境稳定剂作用机制的不同方面。

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