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多发性硬化症中的丘脑损伤与认知

Thalamic Injury and Cognition in Multiple Sclerosis.

作者信息

Amin Moein, Ontaneda Daniel

机构信息

Neurological Institute, Cleveland Clinic, Cleveland, OH, United States.

Mellen Center for Multiple Sclerosis Treatment and Research, Neurological Institute, Cleveland Clinic, Cleveland, OH, United States.

出版信息

Front Neurol. 2021 Feb 5;11:623914. doi: 10.3389/fneur.2020.623914. eCollection 2020.

Abstract

Multiple sclerosis (MS) produces demyelination and degeneration in both gray and white matter. Both cortical and deep gray matter injury is observed during the course of MS. Among deep gray matter structures, the thalamus has received special attention, as it undergoes volume loss in different MS subtypes and is involved in the earliest form of the disease, radiologically isolated syndrome. The thalamus plays an important role as an information relay center, and involvement of the thalamus in MS has been associated with a variety of clinical manifestations in MS, including fatigue, movement disorders, pain, and cognitive impairment (CI). Similar to thalamic volume loss, CI is seen from the earliest stages of MS and is potentially one of the most debilitating manifestations of the disease. The thalamus, particularly the dorsomedial nucleus as part of the basolateral limbic circuit and anterior thalamic nuclei through connections with the prefrontal cortex, has been shown to be involved in CI. Specifically, several cognitive performance measures such as processing speed and memory correlate with thalamic volume. Thalamic atrophy is one of the most important predictors of CI in MS, and both thalamic volume, diffusion tensor imaging measures, and functional activation correlate with the degree of CI in MS. Although the exact mechanism of thalamic atrophy is not well-understood, it is hypothesized to be secondary to degeneration following white matter injury resulting in secondary neurodegeneration and neuronal loss. The thalamus may represent an ideal biomarker for studies aiming to test neuroprotective or restorative therapies aimed at cognition.

摘要

多发性硬化症(MS)会导致灰质和白质的脱髓鞘及变性。在MS病程中可观察到皮质和深部灰质均受损。在深部灰质结构中,丘脑受到了特别关注,因为它在不同的MS亚型中会出现体积缩小,且与疾病的最早形式——放射学孤立综合征有关。丘脑作为信息中继中心发挥着重要作用,丘脑受累与MS的多种临床表现相关,包括疲劳、运动障碍、疼痛和认知障碍(CI)。与丘脑体积缩小类似,CI在MS的最早阶段就会出现,并且可能是该疾病最使人衰弱的表现之一。丘脑,特别是作为基底外侧边缘回路一部分的背内侧核以及通过与前额叶皮质的连接的前丘脑核,已被证明与CI有关。具体而言,一些认知表现指标,如处理速度和记忆力,与丘脑体积相关。丘脑萎缩是MS中CI最重要的预测指标之一,丘脑体积、扩散张量成像测量以及功能激活均与MS中的CI程度相关。尽管丘脑萎缩的确切机制尚未完全明确,但据推测是继发于白质损伤后的变性,导致继发性神经变性和神经元丢失。丘脑可能是旨在测试针对认知的神经保护或恢复性疗法的研究的理想生物标志物。

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