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正在研发的用于抑制肌萎缩侧索硬化症中运动神经元过度兴奋的新型疗法。

Novel therapies in development that inhibit motor neuron hyperexcitability in amyotrophic lateral sclerosis.

作者信息

Noto Yu-Ichi, Shibuya Kazumoto, Vucic Steve, Kiernan Matthew C

机构信息

a Brain and Mind Centre and Sydney Medical School , University of Sydney , Sydney , Australia.

b Westmead Clinical School , University of Sydney , Sydney , Australia.

出版信息

Expert Rev Neurother. 2016 Oct;16(10):1147-54. doi: 10.1080/14737175.2016.1197774. Epub 2016 Jun 17.

Abstract

INTRODUCTION

Motor neuron hyperexcitability appears linked to the process of neurodegeneration in amyotrophic lateral sclerosis (ALS). As such, therapies that inhibit neuronal hyperexcitability may prove effective in arresting the progression of ALS.

AREA COVERED

We searched MEDLINE and ClinicalTrials.gov and selected randomised controlled trials that covered neuroprotective therapy. Riluzole has been established to reduce neuronal hyperexcitability. More recently, initial studies of Na(+) channel blockers (mexiletine and flecainide) have been trialled. Separately, a trial of a K(+) channel activator (retigabine) is underway, while edaravone is currently being considered for licensing by drug approval agencies based on a hypothesis that the elimination of free radicals may lead to protection of motor neurones. Expert commentary: Initial clinical trials with Na(+) channel blockers have not yet established efficacy in ALS. Currently, retigabine is under evaluation as a potential therapy. Edaravone has recently been approved as a new therapeutic option for ALS in Japan.

摘要

引言

运动神经元兴奋性过高似乎与肌萎缩侧索硬化症(ALS)的神经退行性变过程相关。因此,抑制神经元兴奋性过高的疗法可能对阻止ALS的进展有效。

涵盖领域

我们检索了MEDLINE和ClinicalTrials.gov,并选择了涵盖神经保护疗法的随机对照试验。已证实利鲁唑可降低神经元兴奋性过高。最近,对钠通道阻滞剂(美西律和氟卡尼)的初步研究已进行了试验。另外,一项钾通道激活剂(瑞替加滨)的试验正在进行中,而依达拉奉目前正基于自由基清除可能导致运动神经元保护的假说,被药物审批机构考虑授予许可。专家评论:钠通道阻滞剂的初步临床试验尚未证实其对ALS有效。目前,瑞替加滨正在作为一种潜在疗法进行评估。依达拉奉最近在日本已被批准作为ALS的一种新治疗选择。

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