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视神经炎作为多发性硬化症神经保护治疗的2期范例:当前试验及前景的最新进展

Optic neuritis as a phase 2 paradigm for neuroprotection therapies of multiple sclerosis: update on current trials and perspectives.

作者信息

Aktas Orhan, Albrecht Philipp, Hartung Hans-Peter

机构信息

Department of Neurology, Medical Faculty, Heinrich Heine University Düsseldorf, Germany.

出版信息

Curr Opin Neurol. 2016 Jun;29(3):199-204. doi: 10.1097/WCO.0000000000000327.

Abstract

PURPOSE OF REVIEW

In multiple sclerosis as the most common inflammatory demyelinating disease in Western countries, major therapeutic success has been achieved with regard to strategies targeting immunological master switches. These approaches effectively reduce inflammatory disease activity but fail to address ongoing neurodegeneration or disturbed regeneration. However, intense research efforts investigating molecular mechanisms of disease have identified 'druggable' targets for prevention of inflammatory neurodegeneration and disturbed regeneration. This review covers recent developments in clinical trials using optic neuritis as a model for screening such neuroprotective and neuroregenerative therapeutic approaches.

RECENT FINDINGS

Optic neuritis has been used in a series of recent pilot studies investigating the effects of erythropoietin, simvastatin, autologous mesenchymal stem cells, phenytoin, as well as blockade of LINGO-1 (opicinumab). Of note, these studies applied novel outcome measures related to function and structure of the visual pathway, including optical coherence tomography, full-field visual-evoked potentials, multifocal visual-evoked potential, high as well as low-contrast visual acuity. Comparison of these different approaches reveals novel insights into short-term evolution of neurobiological effects during optic neuritis and the window of opportunity for therapeutic interventions.

SUMMARY

Translation of neuroprotective and neuroregenerative approaches to clinical reality represents a huge challenge. Optic neuritis as a prototypic autoimmune demyelinating disease offers an option for testing new therapies targeting key deleterious processes in multiple sclerosis.

摘要

综述目的

在西方国家,多发性硬化作为最常见的炎性脱髓鞘疾病,针对免疫主开关的治疗策略已取得重大成功。这些方法有效降低了炎性疾病活动,但未能解决持续的神经退行性变或再生障碍问题。然而,对疾病分子机制的深入研究已确定了预防炎性神经退行性变和再生障碍的“可药物化”靶点。本综述涵盖了以视神经炎为模型筛选此类神经保护和神经再生治疗方法的临床试验的最新进展。

最新发现

在最近一系列的初步研究中,视神经炎被用于研究促红细胞生成素、辛伐他汀、自体间充质干细胞、苯妥英钠以及LINGO-1阻断剂(opicinumab)的作用。值得注意的是,这些研究采用了与视觉通路功能和结构相关的新结局指标,包括光学相干断层扫描、全视野视觉诱发电位、多焦视觉诱发电位、高对比度和低对比度视力。对这些不同方法的比较揭示了对视神经炎期间神经生物学效应短期演变以及治疗干预机会窗口的新见解。

总结

将神经保护和神经再生方法转化为临床实际应用面临巨大挑战。视神经炎作为一种典型的自身免疫性脱髓鞘疾病,为测试针对多发性硬化关键有害过程的新疗法提供了一个选择。

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