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Recent Clinical Advances in Pharmacotherapy for Levodopa-Induced Dyskinesia

机译:左旋多巴诱导的止吐剂药物治疗临床研究进展

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Onset of involuntary movement patterns of the face, body and limbs are known as dyskinesia. They mostly appear in association with long-term levodopa (l-dopa) therapy in patients with Parkinson's disease. Consequences include patient distress, caregiver embarrassment and reduced quality of life. A severe intensity of this motor complication may result in troublesome disability; however, patients typically prefer motor behaviour with slight, non-troublesome dyskinesia to 'OFF' states. Pharmacotherapy of dyskinesia is complex. Continuous nigrostriatal postsynaptic dopaminergic receptor stimulation may delay onset of l-dopa-associated dyskinesia, while non-physiological, 'pulsatile' receptor stimulation facilitates appearance of dyskinesia. In the past, there have been many clinical trial failures with compounds that were effective in animal models of dyskinesia. Only the N-methyl-d-aspartate antagonist amantadine has shown moderate antidyskinetic effects in small well-designed clinical studies. Amantadine is an old antiviral compound, which moderately improves impaired motor behaviour. Recently, there has been a resurgence of its use due to the US Food and Drug Administration approval of an extended-release (ER) amantadine formulation for treatment of l-dopa-induced dyskinesia. This pharmacokinetic innovation improved dyskinesia and 'OFF' states in pivotal trials, with a once-daily oral application in the evening. Amantadine ER provides higher and more continuous amantadine plasma bioavailability than conventional immediate-release formulations, which require administration up to three times daily.
机译:面部,身体和肢体的非自愿运动模式发作称为障碍血症。它们主要与帕金森病患者的长期左司(L-DOPA)治疗相关联。后果包括患者痛苦,照顾者尴尬和降低的生活质量。这种电动机并发症的严重强度可能导致残疾人麻烦;然而,患者通常更喜欢轻微,非麻烦的动力行为,无疑是“关闭”状态。药物治疗障碍症是复杂的。连续的硝基睾丸突触后的多巴胺能受体受体刺激可能会延迟L-DOPA相关的止吐剂瘤,而非生理的'脉动'受体刺激促进止吐剂的外观。过去,许多临床试验失败与止吐剂的动物模型有效的化合物。只有N-甲基-D-天冬氨酸拮抗剂氨基胺显示在小型精心设计的临床研究中的中度抗菌作用。 Amantadine是一种旧的抗病毒化合物,适度地提高了运动行为受损。最近,由于美国食品和药物管理局批准延长释放(ER)纯草甘化制剂的使用,以治疗L-DOPA诱导的止吐剂的延长的使用,这是一种重新训练。这种药代动力学创新改善了痛经和枢轴试验中的州,晚上每日一次口服申请。氨基氨基ER提供比常规立即释放制剂更高,更常见的纯血浆生物利用度,其每天需要施用3次。

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