Department of Clinical Neurosciences, UCL Institute of Neurology, London, UK.
CNS Drugs. 2011 Dec 1;25(12):1061-71. doi: 10.2165/11596310-000000000-00000.
Parkinson's disease is a disorder characterized pathologically by progressive neurodegeneration of the dopaminergic cells of the nigrostriatal pathway. Although the resulting dopamine deficiency is the cause of the typical motor features of Parkinson's disease (bradykinesia, rigidity, tremor), additional non-motor symptoms appear at various timepoints and are the result of non-dopamine nerve degeneration. Monoamine oxidase B (MAO-B) inhibitors are used in the symptomatic treatment of Parkinson's disease as they increase synaptic dopamine by blocking its degradation. Two MAO-B inhibitors, selegiline and rasagiline, are currently licensed in Europe and North America for the symptomatic improvement of early Parkinson's disease and to reduce off-time in patients with more advanced Parkinson's disease and motor fluctuations related to levodopa. A third MAO-B inhibitor (safinamide), which also combines additional non-dopaminergic properties of potential benefit to Parkinson's disease, is currently under development in phase III clinical trials as adjuvant therapy to either a dopamine agonist or levodopa. MAO-B inhibitors have also been studied extensively for possible neuroprotective or disease-modifying actions. There is considerable laboratory evidence that MAO-B inhibitors do exert some neuroprotective properties, at least in the Parkinson's disease models currently available. However, these models have significant limitations and caution is required in assuming that such results may easily be extrapolated to clinical trials. Rasagiline 1 mg/day has been shown to provide improved motor control in terms of Unified Parkinson's Disease Rating Scale (UPDRS) score at 18 months in those patients with early disease who began the drug 9 months before a second group. There are a number of possible explanations for this effect that may include a disease-modifying action; however, the US FDA recently declined an application for the licence of rasagiline to be extended to cover disease modification.
帕金森病是一种以黑质纹状体通路多巴胺能神经元进行性退化为特征的疾病。虽然多巴胺的缺乏是导致帕金森病典型运动症状(运动迟缓、僵直、震颤)的原因,但在不同时间点还会出现其他非运动症状,这些症状是由于非多巴胺能神经退化引起的。单胺氧化酶 B(MAO-B)抑制剂被用于帕金森病的症状治疗,因为它们通过阻断多巴胺的降解来增加突触中的多巴胺。目前,在欧洲和北美,有两种 MAO-B 抑制剂(司来吉兰和雷沙吉兰)被批准用于早期帕金森病的症状改善,并减少运动波动与左旋多巴相关的晚期帕金森病患者的停药时间。第三种 MAO-B 抑制剂(沙芬酰胺)也具有其他非多巴胺能特性,可能对帕金森病有益,目前正在进行 III 期临床试验,作为多巴胺激动剂或左旋多巴的辅助治疗。MAO-B 抑制剂也被广泛研究用于可能的神经保护或疾病修饰作用。有大量的实验室证据表明,MAO-B 抑制剂确实具有一定的神经保护特性,至少在目前可用的帕金森病模型中是如此。然而,这些模型存在显著的局限性,因此在假设这些结果可能很容易外推到临床试验时需要谨慎。在那些疾病早期的患者中,每天服用 1 毫克雷沙吉兰可在 18 个月时通过统一帕金森病评定量表(UPDRS)评分改善运动控制,这些患者在开始服用药物的 9 个月前就进入了另一组。对于这种效果,可能有许多种解释,包括疾病修饰作用;然而,美国 FDA 最近拒绝了将雷沙吉兰的许可范围扩大到疾病修饰的申请。
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