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多次小剂量左旋多巴加恩他卡朋可产生持续的多巴胺能刺激,并减少经1-甲基-4-苯基-1,2,3,6-四氢吡啶(MPTP)处理的未用过药的灵长类动物的异动症诱发。

Multiple small doses of levodopa plus entacapone produce continuous dopaminergic stimulation and reduce dyskinesia induction in MPTP-treated drug-naive primates.

作者信息

Smith Lance A, Jackson Michael J, Al-Barghouthy Ghassan, Rose Sarah, Kuoppamaki Mikko, Olanow Warren, Jenner Peter

机构信息

Neurodegenerative Diseases Research Centre, GKT School of Biomedical Sciences, King's College, London, United Kingdom.

出版信息

Mov Disord. 2005 Mar;20(3):306-14. doi: 10.1002/mds.20317.

Abstract

Long-acting dopamine agonist drugs induce a lower incidence of dyskinesia in MPTP-treated primates and patients with Parkinson's disease compared to pulsatile treatment with levodopa, supporting the concept of continuous dopaminergic stimulation as a means of dyskinesia avoidance. We examined the effects of L-dopa administered with or without the COMT inhibitor entacapone on dyskinesia induction in previously untreated MPTP-treated common marmosets. Administration of L-dopa (12.5 mg/kg p.o.) plus carbidopa twice daily produced fluctuating improvement in motor behavior coupled with dyskinesia. Coadministration with entacapone produced similar patterns of motor improvement and dyskinesia that were not different from that produced by L-dopa alone. Treatment with L-dopa (6.25 mg/kg p.o.) plus carbidopa four times daily reversed motor disability and induced dyskinesia in a manner that was not different from the twice-daily treatment regimens. However, coadministration with entacapone produced more continuous improvement in locomotor activity with less dyskinesia than animals treated with L-dopa four times daily alone. These data support the notion that pulsatile stimulation contributes to the development of dyskinesia and suggests that more frequent dosing of L-dopa plus entacapone may be a useful treatment strategy for patients in the early stages of Parkinson's disease.

摘要

与左旋多巴脉冲治疗相比,长效多巴胺激动剂药物在MPTP处理的灵长类动物和帕金森病患者中诱发运动障碍的发生率较低,这支持了持续多巴胺能刺激作为避免运动障碍的一种方式的概念。我们研究了在先前未经治疗的MPTP处理的普通狨猴中,给予左旋多巴加或不加儿茶酚-O-甲基转移酶(COMT)抑制剂恩他卡朋对运动障碍诱导的影响。每日两次口服左旋多巴(12.5mg/kg)加卡比多巴可使运动行为出现波动改善并伴有运动障碍。与恩他卡朋联合给药产生的运动改善和运动障碍模式与单独使用左旋多巴产生的相似。每日四次口服左旋多巴(6.25mg/kg)加卡比多巴可逆转运动功能障碍并诱发运动障碍,其方式与每日两次治疗方案无异。然而,与恩他卡朋联合给药比单独每日四次给予左旋多巴治疗的动物在运动活动方面产生更持续的改善且运动障碍更少。这些数据支持了脉冲刺激促成运动障碍发展的观点,并表明更频繁地给予左旋多巴加恩他卡朋可能是帕金森病早期患者的一种有用治疗策略。

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