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恩他卡朋治疗帕金森病

Entacapone in the treatment of Parkinson's disease.

作者信息

Schrag Anette

机构信息

University Department of Clinical Neurosciences, Royal Free and University College Medical School, London, UK.

出版信息

Lancet Neurol. 2005 Jun;4(6):366-70. doi: 10.1016/S1474-4422(05)70098-3.

Abstract

BACKGROUND

The development of fluctuations in motor response and involuntary movements commonly complicate the treatment of Parkinson's disease (PD). Catechol-O-methyltransferase (COMT) inhibitors delay the breakdown of levodopa, which leads to an increase in levodopa bioavailability and more stable concentrations of plasma levodopa. The addition of a COMT inhibitor therefore combines the rapid onset of levodopa with prolonged efficacy, and theoretically provides a more continuous stimulation of dopamine receptors with reduced risk of motor complications. Randomised, controlled trials have shown that in patients with PD who have motor fluctuations, the addition of the COMT-inhibitor entacapone results in an improvement in motor fluctuations, particularly of the "wearing-off" type, with about 1.0-1.7 h more on-time and less off-time per day, reduced required levodopa dose, modest improvement in motor and disability scores (mean total unified PD rating scale [UPDRS] scores of about 4.5), and in some but not all studies improvement of health-related quality of life [HRQOL] scores.

RECENT DEVELOPMENTS

Patients with stable PD, without motor fluctuations, also have improved HRQOL scores on treatment with entacapone in addition to levodopa with a dopa-decarboxylase inhibitor. However, in a recent large multicentre study, UPDRS motor and disability scores were not improved despite significant improvements in HRQOL scores. The disparity between results on clinical rating scales and HRQOL scores suggests that these scales give different and potentially complementary information on health status changes in PD, and that entacapone provides benefit that may not be captured with standard clinical rating scales. Whether entacapone combined with levodopa can delay dyskinesia or motor fluctuations in patients with untreated PD is unknown; however, in animal studies, a decrease in motor complications has been reported in drug-naive animals given frequent doses of levodopa combined with entacapone. WHERE NEXT?: Clinical studies are underway to address the hypothesis that motor complications in PD can be delayed if entacapone is given from the start of treatment. Until the results of these trials are available, entacapone is indicated as a useful adjunct to levodopa in the symptomatic treatment of patients with PD with and without motor fluctuations. In addition, future trials should specifically assess the effect of entacapone on HRQOL in PD.

摘要

背景

运动反应波动和不自主运动的出现通常会使帕金森病(PD)的治疗变得复杂。儿茶酚-O-甲基转移酶(COMT)抑制剂可延缓左旋多巴的分解,从而导致左旋多巴生物利用度增加以及血浆左旋多巴浓度更稳定。因此,添加COMT抑制剂可使左旋多巴起效迅速且疗效持久,理论上能更持续地刺激多巴胺受体,降低运动并发症风险。随机对照试验表明,在有运动波动的PD患者中,添加COMT抑制剂恩他卡朋可改善运动波动,尤其是“剂末现象”型,每天的“开”期时间增加约1.0 - 1.7小时,“关”期时间减少,左旋多巴剂量需求降低,运动和残疾评分有适度改善(统一PD评定量表[UPDRS]总分平均约提高4.5分),并且在部分但并非所有研究中,健康相关生活质量(HRQOL)评分也有所改善。

最新进展

病情稳定、无运动波动的PD患者,在左旋多巴与多巴脱羧酶抑制剂联合治疗的基础上加用恩他卡朋后,HRQOL评分也有所提高。然而,在最近一项大型多中心研究中,尽管HRQOL评分有显著改善,但UPDRS运动和残疾评分并未提高。临床评定量表结果与HRQOL评分之间的差异表明,这些量表在PD健康状况变化方面提供了不同且可能互补的信息,并且恩他卡朋带来的益处可能无法通过标准临床评定量表体现。恩他卡朋联合左旋多巴能否延缓未治疗PD患者的异动症或运动波动尚不清楚;不过,在动物研究中,频繁给予左旋多巴联合恩他卡朋的未用药动物的运动并发症有所减少。

下一步方向

正在进行临床研究以验证从治疗开始就给予恩他卡朋是否能延缓PD运动并发症这一假设。在这些试验结果出来之前,恩他卡朋被认为是对有或无运动波动的PD患者进行症状性治疗时左旋多巴的有用辅助药物。此外,未来试验应专门评估恩他卡朋对PD患者HRQOL的影响。

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