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Parkinson’s disease, L-DOPA, and endogenous morphine: A revisit

机译:帕金森氏病,L-DOPA和内源性吗啡:回顾

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摘要

Clinical observations stemming from widespread employment of restorative L-3,4-dihydroxyphenylalanine (L-DOPA) therapy for management of dyskinesia in Parkinson’s Disease (PD) patients implicate a regulatory role for endogenous morphine in central nervous system dopamine neurotransmission. Reciprocally, it appears that restorative L-DOPA administration has provided us with a compelling in vivo pharmacological model for targeting peripheral sites involved in endogenous morphine expression in human subjects. The biological activities underlying endogenous morphine expression and its interaction with its major precursor dopamine strongly suggest that endogenous morphine systems are reciprocally dysregulated in PD. These critical issues are examined from historical and current perspectives within our short review.
机译:在帕金森病(PD)患者中广泛使用恢复性L-3,4-二羟基苯丙氨酸(L-DOPA)治疗运动障碍所产生的临床观察表明,内源性吗啡在中枢神经系统多巴胺神经传递中起调节作用。相应地,看来恢复性L-DOPA给药已为我们提供了一种引人注目的体内药理模型,可用于靶向涉及人类受试者内源性吗啡表达的外围位点。内源性吗啡表达及其与其主要前体多巴胺的相互作用所具有的生物学活性强烈表明,内源性吗啡系统在PD中相互失调。在我们的简短回顾中,从历史和当前的角度对这些关键问题进行了研究。

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