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Parkinson’s Disease: Low-Dose Haloperidol Increases Dopamine Receptor Sensitivity and Clinical Response

机译:帕金森氏病:低剂量氟哌啶醇可提高多巴胺受体的敏感性和临床反应

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Background. It is known that ultra-low doses of haloperidol can cause dopamine supersensitivity of dopamine D2 receptors and related behaviour in animals. Objective. The objective was to determine whether a daily ultra-low dose of 40 micrograms of haloperidol could enhance the clinical action of levodopa in Parkinson’s disease patients. Method. While continuing their daily treatment with levodopa, 16 patients with Parkinson’s disease were followed weekly for six weeks. They received an add-on daily dose of 40 micrograms of haloperidol for the first two weeks only. The SPES/SCOPA scale (short scale for assessment of motor impairments and disabilities in Parkinson’s disease) was administered before treatment and weekly throughout the trial. Results. The results showed a mean decrease in SPES/SCOPA scores after one week of the add-on treatment. Conclusion. SCOPA scores decreased after the addition of low-dose haloperidol to the standard daily levodopa dose. This finding is consistent with an increase in sensitivity of dopamine D2 receptors induced by haloperidol. Such treatment for Parkinson’s disease may possibly permit the levodopa dose to be reduced and, thus, delay the onset of levodopa side effects.
机译:背景。众所周知,超低剂量的氟哌啶醇会引起多巴胺D2受体的多巴胺超敏性以及动物相关行为。目的。目的是确定每日超低剂量的40微克氟哌啶醇能否增强帕金森氏病患者的左旋多巴的临床作用。方法。在继续每日服用左旋多巴的同时,每周随访16名帕金森氏病患者,持续6周。他们仅在前两周每天接受40克氟哌啶醇的追加剂量。 SPES / SCOPA量表(评估帕金森氏病的运动障碍和残疾的简短量表)在治疗前和试验期间每周进行一次。结果。结果显示,附加治疗一周后,SPES / SCOPA得分平均下降。结论。在标准左旋多巴每日剂量中加入小剂量氟哌啶醇后,SCOPA评分降低。这一发现与氟哌啶醇诱导的多巴胺D2受体敏感性的增加相一致。帕金森氏病的这种治疗方法可能会降低左旋多巴的剂量,从而延迟左旋多巴副作用的发作。

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