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2
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本文引用的文献

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Early combination therapy (bromocriptine and levodopa) does not prevent motor fluctuations in Parkinson's disease.早期联合治疗(溴隐亭和左旋多巴)不能预防帕金森病的运动波动。
Neurology. 1993 Jan;43(1):21-7. doi: 10.1212/wnl.43.1_part_1.21.
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Risk factors for motor response complications in L-dopa-treated parkinsonian patients.左旋多巴治疗帕金森病患者运动反应并发症的危险因素。
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Early combination therapy with bromocriptine and levodopa in Parkinson's disease.帕金森病中溴隐亭与左旋多巴的早期联合治疗。
Mov Disord. 1993 Jul;8(3):257-62. doi: 10.1002/mds.870080302.
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Sustained bromocriptine therapy in previously untreated patients with Parkinson's disease.对既往未经治疗的帕金森病患者进行溴隐亭持续治疗。
J Neurol Neurosurg Psychiatry. 1981 Nov;44(11):1020-3. doi: 10.1136/jnnp.44.11.1020.
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Combined bromocriptine-levodopa therapy early in Parkinson's disease.帕金森病早期联合使用溴隐亭-左旋多巴疗法。
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Early combination of bromocriptine and levodopa in the treatment of Parkinson's disease: a 5-year follow-up.溴隐亭与左旋多巴早期联合治疗帕金森病:5年随访
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一项随机对照研究,比较了先使用溴隐亭随后加用左旋多巴的治疗方案与单独使用左旋多巴治疗方案,用于治疗既往未接受治疗的帕金森病患者:五年随访。

A randomised controlled study comparing bromocriptine to which levodopa was later added, with levodopa alone in previously untreated patients with Parkinson's disease: a five year follow up.

作者信息

Montastruc J L, Rascol O, Senard J M, Rascol A

机构信息

Department of Medical and Clinical Pharmacology, Inserm U 317, Toulouse, France.

出版信息

J Neurol Neurosurg Psychiatry. 1994 Sep;57(9):1034-8. doi: 10.1136/jnnp.57.9.1034.

DOI:10.1136/jnnp.57.9.1034
PMID:8089666
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1073123/
Abstract

This pilot study was performed to compare the occurrence of long term motor complications in Parkinson's disease when the introduction of levodopa was delayed by an initial treatment with high doses of bromocriptine alone. The trial was a prospective randomised controlled study comparing 31 previously untreated patients with Parkinson's disease initially given bromocriptine alone to which levodopa was later added (group B/D) and 29 other previously untreated patients with Parkinson's disease immediately given levodopa alone (group D). The end point was the occurrence of the first motor complications (wearing off or dyskinesia). Group B/D patients received bromocriptine (52 (SEM 5) mg/day) for 2.7 years, to which levodopa was later added (471 (SEM 46) mg/day). Group D patients received a comparable dose of levodopa alone (569 (SEM 47) mg/day). Both had similar disability scores at the end of the study. Motor complications were fewer and appeared later in group B/D than in group D (56% after 4.9 (SEM 0.5) years of treatment v 90% after 2.7 (SEM 0.5) years, p < 0.01). Wearing off appeared later (p < 0.01) in group B/D (4.5 (SEM 0.6) years) than in group D (2.9 (SEM 0.6) years). Peak dose dyskinesia occurred less often in group B/D patients (three v 14 cases, p < 0.01). This study showed that a three year initial monotherapy with high doses of bromocriptine followed by addition of levodopa delayed the occurrence of long term motor complications usually found in patients with Parkinson's disease treated with levodopa alone from the beginning.

摘要

本前瞻性研究旨在比较帕金森病患者长期运动并发症的发生率,这些患者最初仅接受高剂量溴隐亭治疗,从而延迟左旋多巴的引入。该试验为前瞻性随机对照研究,比较了31例既往未接受治疗的帕金森病患者,这些患者最初仅给予溴隐亭,随后添加左旋多巴(B/D组),以及29例其他既往未接受治疗的帕金森病患者,这些患者立即单独给予左旋多巴(D组)。终点为首次出现运动并发症(疗效减退或异动症)。B/D组患者接受溴隐亭(52(标准误5)mg/天)治疗2.7年,随后添加左旋多巴(471(标准误46)mg/天)。D组患者单独接受相当剂量的左旋多巴(569(标准误47)mg/天)。研究结束时两组的残疾评分相似。B/D组的运动并发症比D组更少且出现更晚(治疗4.9(标准误0.5)年后为56%,而治疗2.7(标准误0.5)年后为90%,p<0.01)。B/D组疗效减退出现更晚(p<0.01)(4.5(标准误0.6)年),而D组为2.9(标准误0.6)年。B/D组患者峰值剂量异动症的发生率更低(3例对14例,p<0.01)。本研究表明,最初三年采用高剂量溴隐亭单一疗法,随后添加左旋多巴,可延迟帕金森病患者长期运动并发症的出现,这些并发症通常见于从一开始就单独使用左旋多巴治疗的患者。