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多发性硬化症神经退行性阶段的生物学指标。

Biological indicators of the neurodegenerative phase of multiple sclerosis.

作者信息

Zaffaroni M

机构信息

Multiple Sclerosis Study Center, Gallarate Hospital, Via Pastori 4, I-21013, Gallarate (VA), Italy.

出版信息

Neurol Sci. 2003 Dec;24 Suppl 5:S279-82. doi: 10.1007/s10072-003-0174-3.

Abstract

The recent re-discovery of axonal damage in multiple sclerosis has led to a renewed interest in neurodegenerative mechanisms of the disease. Transected or injured axons release several molecules from their proximal extremity into the intercellular space. Although these molecules can be measured, however, a biological marker of axonal and neuronal degeneration is still lacking. Cytoskeleton structural proteins like actin, tubulin, L-neurofilaments and tau protein, axon-specific antibodies, other neuronal or glial proteins like S-100, 14-3-3 and glial fibrillary acid protein, neuronal specific enolase, and nitric oxide and its metabolites are some of the putative markers that deserve further investigation and validation. At present, none of them fulfils the criteria of applicability in clinical practice, and the levels of N-acetylaspartate determined by magnetic resonance spectroscopy remain the most reliable measure of axonal damage.

摘要

近期在多发性硬化症中重新发现轴突损伤,引发了人们对该疾病神经退行性机制的新兴趣。横断或受损的轴突会从其近端向细胞间空间释放多种分子。然而,尽管这些分子能够被检测出来,但轴突和神经元变性的生物学标志物仍然缺失。细胞骨架结构蛋白,如肌动蛋白、微管蛋白、L-神经丝和tau蛋白,轴突特异性抗体,其他神经元或神经胶质蛋白,如S-100、14-3-3和胶质纤维酸性蛋白,神经元特异性烯醇化酶,以及一氧化氮及其代谢产物,都是一些值得进一步研究和验证的假定标志物。目前,它们中没有一个符合临床实践中的适用性标准,而通过磁共振波谱测定的N-乙酰天门冬氨酸水平仍然是轴突损伤最可靠的测量指标。

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