Multiple Sclerosis and Aging: The Dynamics of Demyelination and Remyelination.

IF 3.9 4区 医学 Q2 NEUROSCIENCES ASN NEURO Pub Date : 2022-01-01 DOI:10.1177/17590914221118502
Jorge Correale, Maria Celica Ysrraelit
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引用次数: 7

Abstract

Multiple sclerosis (MS) is a chronic inflammatory disease of the central nervous system (CNS) leading to demyelination and neurodegeneration. Life expectancy and age of onset in MS patients have been rising over the last decades, and previous studies have shown that age affects disease progression. Therefore, age appears as one of the most important factors in accumulating disability in MS patients. Indeed, the degeneration of oligodendrocytes (OGDs) and OGD precursors (OPCs) increases with age, in association with increased inflammatory activity of astrocytes and microglia. Similarly, age-related neuronal changes such as mitochondrial alterations, an increase in oxidative stress, and disrupted paranodal junctions can impact myelin integrity. Conversely, once myelination is complete, the long-term integrity of axons depends on OGD supply of energy. These alterations determine pathological myelin changes consisting of myelin outfolding, splitting, and accumulation of multilamellar fragments. Overall, these data demonstrate that old mature OGDs lose their ability to produce and maintain healthy myelin over time, to induce de novo myelination, and to remodel pre-existing myelinated axons that contribute to neural plasticity in the CNS. Furthermore, as observed in other tissues, aging induces a general decline in regenerative processes and, not surprisingly, progressively hinders remyelination in MS. In this context, this review will provide an overview of the current knowledge of age-related changes occurring in cells of the oligodendroglial lineage and how they impact myelin synthesis, axonal degeneration, and remyelination efficiency.

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多发性硬化症和衰老:脱髓鞘和再生的动态。
多发性硬化症(MS)是中枢神经系统(CNS)的慢性炎症性疾病,导致脱髓鞘和神经变性。在过去的几十年里,多发性硬化症患者的预期寿命和发病年龄一直在上升,以前的研究表明年龄影响疾病的进展。因此,年龄是MS患者残疾积累的最重要因素之一。事实上,少突胶质细胞(OGDs)和OGD前体(OPCs)的退化随着年龄的增长而增加,与星形胶质细胞和小胶质细胞的炎症活性增加有关。同样,与年龄相关的神经元变化,如线粒体改变、氧化应激增加和旁神经连接破坏,也会影响髓磷脂的完整性。相反,一旦髓鞘形成完成,轴突的长期完整性依赖于OGD的能量供应。这些改变决定了髓磷脂的病理改变,包括髓磷脂外折叠、分裂和多层碎片的积累。总的来说,这些数据表明,随着时间的推移,年老的成熟ogd失去了产生和维持健康髓磷脂的能力,从而诱导新生髓鞘形成,并重塑先前存在的髓鞘轴突,从而促进中枢神经系统的神经可塑性。此外,正如在其他组织中观察到的那样,衰老会导致再生过程的普遍下降,并逐渐阻碍ms的髓鞘再生,这并不奇怪。在此背景下,本综述将概述当前对少突胶质细胞谱系中发生的年龄相关变化的了解,以及它们如何影响髓鞘合成、轴突变性和髓鞘再生效率。
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来源期刊
ASN NEURO
ASN NEURO NEUROSCIENCES-
CiteScore
7.70
自引率
4.30%
发文量
35
审稿时长
>12 weeks
期刊介绍: ASN NEURO is an open access, peer-reviewed journal uniquely positioned to provide investigators with the most recent advances across the breadth of the cellular and molecular neurosciences. The official journal of the American Society for Neurochemistry, ASN NEURO is dedicated to the promotion, support, and facilitation of communication among cellular and molecular neuroscientists of all specializations.
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