Pergolide compared with bromocriptine in Parkinson's disease: A multicenter, crossover, controlled study

Pezzoli, Gianni; Martignoni, E.; Pacchetti, Claudio; Angeleri, V. A.; Lamberti, P.; Muratorio, A; Bonuccelli, Ubaldo; Mari, Michele; Foschi, Nazario; Cossutta, E.; Nicoletti, F; Giammona, F.; Canesi, Margherita; Scarlato, G.; Caraceni, T.; Moscarelli, E

doi:10.1002/mds.870090409

Cited by 70 publications

(25 citation statements)

References 20 publications

(4 reference statements)

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“…[73,85,116] However, such data do not have a strong impact on clinical practice because most studies had methodological problems (insufficient power, surrogate endpoints, arbitrary definition of dose equivalences, among others) and reported only modest inter-group differences, posing the question of their relevance in clinical practice. This applies to trials with cabergoline, [94] lisuride, [117,118] pergolide, [63,97,119] pramipexole, [101] piribedil [99] and ropinirole. [110] Bromocriptine [120] and pergolide [121] have been the sole DAs compared with the COMT inhibitor tolcapone in open-label clinical studies, without significant differences in terms of efficacy on the parkinsonian cardinal signs.…”

Section: Symptomatic Control Of Parkinsonian Symptoms In Early Parkinmentioning

confidence: 99%

Dopamine Receptor Agonists for the Treatment of Early or Advanced Parkinsonʼs Disease

2010

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Dopamine receptor agonists are indicated for the symptomatic treatment of early, moderate or advanced Parkinson's disease as well as for the reduction of levodopa-related motor complications. Ergolinic dopamine agonists, such as bromocriptine or pergolide, were initially developed and marketed, and then non-ergolinic dopamine agonists, such as pramipexole and ropinirole, were introduced, reducing the risk of drug-induced fibrotic reactions. Once-daily, controlled-release oral and transdermal formulations have been developed aiming at providing more stable 24-hour plasma drug concentrations and more convenient administration. A disease-modifying effect of dopamine agonists has not been demonstrated clinically. As with any other drug, dopamine agonists can also cause adverse drug reactions, which can be related or unrelated to dopaminergic hyperactivation. Dopaminergic reactions include nausea, hallucinations, confusion and orthostatic hypotension, among others, which were readily identified in pre-marketing clinical trials. During post-marketing surveillance, important adverse reactions were identified, such as daytime somnolence, impulse-control disorders and heart valve fibrosis. Other issues, including the efficacy of dopamine agonists for the treatment of non-motor symptoms, remain under evaluation.

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Section: Symptomatic Control Of Parkinsonian Symptoms In Early Parkinmentioning

confidence: 99%

Dopamine Receptor Agonists for the Treatment of Early or Advanced Parkinsonʼs Disease

2010

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“…Although levodopa is the most common treatment for the relief of symptoms in PD, other treatment regimens have incorporated various direct dopamine agonists, for example apomorphine, [13] and the ergot derivatives pergolide, [14,15] cabergoline, [16]lisuride [17] and bromocriptine. [18] Unfortunately, these agents have limited value because they also elicit dyskinesias when given either with low dosages of levodopa or when given alone to patients previously treated with levodopa.…”

Section: Dyskinesias In Parkinson's Diseasementioning

confidence: 99%

Potential of Opioid Antagonists in the Treatment of Levodopa-Induced Dyskinesias in Parkinson??s Disease

Henry

Brotchie

1996

Drugs & Aging

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Current treatments for Parkinson's disease (PD) rely on dopamine-replacing strategies, and centre around dopamine precursors (e.g. levodopa) or directly acting dopamine agonists. With long-term therapy these agents lose much of their clinical utility due to the appearance of adverse effects such as dyskinesias and/or a wearing off of efficacy. Although dyskinesias in Huntington's disease, hemiballism and experimental animals are thought to be associated with reductions in amino acid transmission within the lateral and medial segments of the globus pallidus, the neural mechanisms underlying treatment-related dyskinesias in PD are poorly understood. Recent evidence suggests that, within these regions of the brain, the opioid peptides enkephalin and dynorphin, acting at delta and kappa opioid receptors, respectively, can reduce the release of amino acid transmitters. Furthermore, the synthesis of these peptides appears to be enhanced in neurons projecting to the pallidal complex in animal models of PD following repeated treatment with dopamine-replacing agents that also cause dyskinetic adverse effects (e.g. levodopa and apomorphine). In contrast, dopamine receptor agonists such as bromocriptine and lisuride do not cause dyskinetic adverse effects following long-term treatment, and do not elevate peptide synthesis when given de novo. These data, together with recent data on the behavioural effects of opioid antagonists in a rodent model of levodopa-induced dyskinesia in PD, suggest the possibility that antagonists of opioid receptors may prove useful as adjuncts to levodopa. By limiting the severity of dyskinetic adverse effects, these drugs may help extend the time for which the antiparkinsonian effects of such compounds can be usefully exploited.

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“…There is some evidence that pergolide is more effective and better tolerated than bromocriptine. 75 Attention to gastric and dietary factors also becomes important. Dissolving levodopa in liquid before ingestion may help,76 as may the use of the dispersible Madopar preparations, which act more quickly.…”

Section: Fluctuationsmentioning

confidence: 99%

Parkinson's disease.

Marsden¹

1994

Journal of Neurology, Neurosurgery & Psychiatry

361

153

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Pergolide compared with bromocriptine in Parkinson's disease: A multicenter, crossover, controlled study

Cited by 70 publications

References 20 publications

Dopamine Receptor Agonists for the Treatment of Early or Advanced Parkinsonʼs Disease

Dopamine Receptor Agonists for the Treatment of Early or Advanced Parkinsonʼs Disease

Potential of Opioid Antagonists in the Treatment of Levodopa-Induced Dyskinesias in Parkinson??s Disease

Parkinson's disease.

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