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运动反应并发症与纹状体传出系统的功能

Motor response complications and the function of striatal efferent systems.

作者信息

Chase T N, Mouradian M M, Engber T M

机构信息

Experimental Therapeutics Branch, National Institute of Neurological Disorders and Stroke, National Institutes of Health, Bethesda, Maryland 20892.

出版信息

Neurology. 1993 Dec;43(12 Suppl 6):S23-7.

PMID:8264907
Abstract

Motor response complications eventually appear in most patients with advanced Parkinson's disease being treated with levodopa. The interval between onset of parkinsonism and emergence of these adverse events appears independent of the dose or the duration of therapy. Current evidence suggests that "wearing-off" fluctuations largely reflect the loss of normally functioning dopaminergic terminals, although postsynaptic alterations contribute somewhat to the underlying decline in the duration of levodopa's antiparkinsonian action. "On-off" fluctuations and peak-dose dyskinesias, on the other hand, appear to arise mainly as a consequence of postjunctional alterations that follow exposure to nonphysiologic intrasynaptic dopamine fluctuations in patients who have lost the buffering afforded by dopaminergic terminals. Studies in rats with 6-hydroxydopamine lesions indicate that striking functional alterations occur in striatal dopaminoceptive systems as a result of dopaminergic denervation and that levodopa replacement, particularly when given intermittently, fails to normalize these changes. To the extent that similar alterations contribute to the appearance of motor complications, the successful symptomatic therapy of Parkinson's disease may require continuous dopaminergic stimulation, as well as direct pharmacologic targeting of striatal dopaminoceptive systems.

摘要

大多数接受左旋多巴治疗的晚期帕金森病患者最终都会出现运动反应并发症。帕金森病发作与这些不良事件出现之间的间隔似乎与治疗剂量或疗程无关。目前的证据表明,“剂末”波动很大程度上反映了正常功能的多巴胺能终末的丧失,尽管突触后改变在一定程度上导致了左旋多巴抗帕金森病作用持续时间的潜在下降。另一方面,“开-关”波动和剂峰异动症似乎主要是由于在失去多巴胺能终末提供的缓冲作用的患者中,暴露于非生理性突触内多巴胺波动后发生的突触后改变所致。对6-羟基多巴胺损伤大鼠的研究表明,多巴胺能去神经支配导致纹状体多巴胺感受系统发生显著的功能改变,左旋多巴替代治疗,尤其是间歇性给药时,无法使这些变化恢复正常。如果类似的改变导致了运动并发症的出现,那么帕金森病的成功对症治疗可能需要持续的多巴胺能刺激,以及对纹状体多巴胺感受系统进行直接的药物靶向治疗。

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