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首页> 外文期刊>Expert opinion on investigational drugs >Remyelinating and neuroprotective treatments in multiple sclerosis.
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Remyelinating and neuroprotective treatments in multiple sclerosis.

机译:多发性硬化症中的髓鞘再生和神经保护治疗。

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摘要

Multiple sclerosis (MS) is the most common cause of neurological disability in young adults. The pathological hallmark is multifocal demyelination and inflammation in the CNS. In addition, there is also a variable extent of axonal damage. Remyelination has been seen in up to 70% of lesions but repair is generally incomplete. The demonstration of neuropathological heterogeneity of MS lesions suggests different pathophysiological subtypes and it is therefore unlikely that there is a uniform cause of incomplete remyelination in MS. In recent years, a great body of knowledge has accumulated in order to better understand the regulatory mechanisms of remyelination. This has led to a number of approaches to promote repair mechanisms, most of which have been successful in animal experiments. Unfortunately, the translation of these experimental data into clinical treatments has proven difficult. More information on the pathogenesis of MS, the reason why repair mechanisms fail in MS and a better understanding ofthe regulation of remyelination are required. This will ultimately lead to a specific treatment tailored for the individual patient and will probably involve a combination of immunomodulation, remyelination and neuroprotection.
机译:多发性硬化症(MS)是年轻人中神经系统残疾的最常见原因。病理特征是中枢神经系统多灶性脱髓鞘和炎症。另外,轴突损伤程度也不同。高达70%的病灶可见髓鞘再生,但修复通常不完全。 MS病变的神经病理学异质性提示不同的病理生理亚型,因此不太可能是造成MS不完全髓鞘化的统一原因。近年来,为了更好地了解髓鞘再生的调控机制,已经积累了大量的知识。这导致了许多促进修复机制的方法,其中大多数已在动物实验中成功。不幸的是,已经证明将这些实验数据转化为临床治疗是困难的。需要更多有关MS发病机理的信息,为什么MS修复机制失败的原因以及对髓鞘再生调节的更好理解。这最终将导致针对个体患者量身定制的特定治疗,并且可能涉及免疫调节,髓鞘再生和神经保护的组合。

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