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多发性硬化症:神经胶质细胞在时间和空间上的多样性

Multiple Sclerosis: Glial Cell Diversity in Time and Space.

作者信息

Kooistra Susanne M, Schirmer Lucas

机构信息

Department of Biomedical Sciences, Section Molecular Neurobiology, University of Groningen and University Medical Center Groningen (UMCG), Groningen, The Netherlands.

Department of Neurology, Medical Faculty Mannheim, Heidelberg University, Mannheim, Germany.

出版信息

Glia. 2025 Mar;73(3):574-590. doi: 10.1002/glia.24655. Epub 2024 Dec 24.

Abstract

Multiple sclerosis (MS) is the most prevalent human inflammatory disease of the central nervous system with demyelination and glial scar formation as pathological hallmarks. Glial cells are key drivers of lesion progression in MS with roles in both tissue damage and repair depending on the surrounding microenvironment and the functional state of the individual glial subtype. In this review, we describe recent developments in the context of glial cell diversity in MS summarizing key findings with respect to pathological and maladaptive functions related to disease-associated glial subtypes. A particular focus is on the spatial and temporal dynamics of glial cells including subtypes of microglia, oligodendrocytes, and astrocytes. We contextualize recent high-dimensional findings suggesting that glial cells dynamically change with respect to epigenomic, transcriptomic, and metabolic features across the inflamed rim and during the progression of MS lesions. In summary, detailed knowledge of spatially restricted glial subtype functions is critical for a better understanding of MS pathology and its pathogenesis as well as the development of novel MS therapies targeting specific glial cell types.

摘要

多发性硬化症(MS)是中枢神经系统最常见的人类炎性疾病,脱髓鞘和胶质瘢痕形成是其病理特征。胶质细胞是MS病变进展的关键驱动因素,根据周围微环境和单个胶质细胞亚型的功能状态,在组织损伤和修复中均发挥作用。在本综述中,我们描述了MS中胶质细胞多样性背景下的最新进展,总结了与疾病相关胶质细胞亚型的病理和适应不良功能相关的关键发现。特别关注胶质细胞的时空动态,包括小胶质细胞、少突胶质细胞和星形胶质细胞的亚型。我们将近期的高维研究结果置于背景中,这些结果表明,在MS病变的炎症边缘及进展过程中,胶质细胞在表观基因组、转录组和代谢特征方面会动态变化。总之,详细了解空间受限的胶质细胞亚型功能对于更好地理解MS病理学及其发病机制以及开发针对特定胶质细胞类型的新型MS疗法至关重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0d05/11784844/88204cd6fc86/GLIA-73-574-g002.jpg

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