多系统萎缩中的神经炎症：对α-突触核蛋白聚集的反应及原因

Neuroinflammation in Multiple System Atrophy: Response to and Cause of α-Synuclein Aggregation.

作者信息

Vieira Bruno Di Marco, Radford Rowan A, Chung Roger S, Guillemin Gilles J, Pountney Dean L

机构信息

Menzies Health Institute Queensland, Griffith University Gold Coast, QLD, Australia.

Department of Biomedical Sciences, Faculty of Medicine and Health Sciences, Macquarie University Sydney, NSW, Australia.

出版信息

Front Cell Neurosci. 2015 Nov 12;9:437. doi: 10.3389/fncel.2015.00437. eCollection 2015.

DOI:10.3389/fncel.2015.00437

PMID:26778958

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4700780/

Abstract

Multiple system atrophy (MSA) is a progressive neurodegenerative disease presenting with combinations of autonomic dysfunction, parkinsonism, cerebellar ataxia and/or pyramidal signs. Oligodendroglial cytoplasmic inclusions (GCIs) rich in α-synuclein (α-syn) constitute the disease hallmark, accompanied by neuronal loss and activation of glial cells which indicate neuroinflammation. Recent studies demonstrate that α-syn may be released from degenerating neurons to mediate formation of abnormal inclusion bodies and to induce neuroinflammation which, interestingly, might also favor the formation of intracellular α-syn aggregates as a consequence of cytokine release and the shift to a pro-inflammatory environment. Here, we critically review the relationships between α-syn and astrocytic and microglial activation in MSA to explore the potential of therapeutics which target neuroinflammation.

摘要

多系统萎缩（MSA）是一种进行性神经退行性疾病，表现为自主神经功能障碍、帕金森综合征、小脑共济失调和/或锥体束征的组合。富含α-突触核蛋白（α-syn）的少突胶质细胞胞质包涵体（GCIs）构成了该疾病的标志，同时伴有神经元丢失和神经胶质细胞激活，提示神经炎症。最近的研究表明，α-syn可能从退化的神经元中释放出来，介导异常包涵体的形成并诱导神经炎症，有趣的是，由于细胞因子释放和向促炎环境的转变，这也可能有利于细胞内α-syn聚集体的形成。在这里，我们批判性地回顾了MSA中α-syn与星形胶质细胞和小胶质细胞激活之间的关系，以探索针对神经炎症的治疗方法的潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/668a/4700780/a7d039bd04b4/fncel-09-00437-g0001.jpg

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多系统萎缩中的神经炎症：对α-突触核蛋白聚集的反应及原因

Neuroinflammation in Multiple System Atrophy: Response to and Cause of α-Synuclein Aggregation.

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