Pergolide
Pergolide is a semisynthetic ergot alkaloid derivative that functions as a potent dopamine receptor agonist, primarily targeting D1 and D2 receptors to mimic the effects of dopamine in the brain.[1][2] Developed for human use in the management of Parkinson's disease as an adjunct to levodopa/carbidopa therapy, it was approved by the FDA in 1988 under the brand name Permax but voluntarily withdrawn from the U.S. market in 2007 and from markets in several other countries due to serious risks of valvular heart disease, though it remains available in some countries.[3][1][4] In veterinary medicine, pergolide remains widely used for treating pituitary pars intermedia dysfunction (PPID), also known as equine Cushing's disease, in horses, where it is marketed as Prascend to regulate hormonal imbalances associated with the condition.[5][6] Pharmacologically, pergolide exhibits high affinity for dopamine receptors, with potency 10 to 100 times greater than that of bromocriptine, another ergot-derived agonist.[2] It is well-absorbed orally, has a plasma half-life of about 21 hours, undergoes hepatic metabolism to active metabolites, and is primarily excreted in urine.[2] In Parkinson's patients, it improves motor symptoms such as bradykinesia and rigidity by directly stimulating dopamine receptors in the substantia nigra and corpus striatum, often reducing "off" periods and end-of-dose deterioration when used adjunctively.[7] Beyond Parkinson's, it has been employed off-label for hyperprolactinemia and prolactinomas, where doses of 0.025 to 0.5 mg/day led to significant tumor shrinkage in over 75% of macroprolactinoma cases.[2] In equine applications, pergolide effectively manages PPID by counteracting dopamine deficiency in the hypothalamus, alleviating clinical signs like hirsutism, laminitis, and muscle wasting.[5] Studies demonstrate improved survival odds and normalized endocrine function in treated horses, with a starting dose of approximately 0.002 mg/kg (2 μg/kg) body weight daily, which may be increased based on response and monitoring.[5][8][9] Recent research also indicates that pergolide can reduce postprandial insulin spikes in PPID-affected horses with concurrent insulin dysregulation, potentially lowering laminitis risk.[10] Common adverse effects in human use include nausea, dizziness, somnolence, and hallucinations, while serious concerns involve cardiac valvulopathy—particularly at doses exceeding 3 mg/day—pleural fibrosis, and rare instances of hepatotoxicity with transient enzyme elevations.[2][1] In horses, side effects are generally mild, such as temporary appetite suppression or depression, but hypersensitivity to ergot derivatives contraindicates its use.[11] Despite its withdrawal for human indications in many countries, pergolide's therapeutic legacy underscores the challenges of balancing dopamine modulation benefits against fibrotic risks in long-term therapy.[3][1]Medical Uses
Human Applications
Pergolide was primarily used as an adjunct therapy to levodopa/carbidopa in the management of motor symptoms associated with advanced Parkinson's disease, particularly in patients experiencing "on-off" fluctuations and dyskinesia.[12] This approach allowed for a reduction in levodopa dosage while maintaining or enhancing clinical outcomes, based on evidence from a multicenter clinical trial involving 376 patients with mild to moderate disease who were intolerant to levodopa/carbidopa due to these complications.[12] Recommended dosing for pergolide in human patients began at 0.05 mg per day for the first two days, followed by gradual titration—increments of 0.1 to 0.15 mg per day every three days for the initial 12 days, then 0.25 mg per day every three days thereafter—until an optimal therapeutic dose was reached.[12] The medication was typically administered in three divided daily doses, with a mean therapeutic dose of 3 mg per day and an average concurrent levodopa dose of 650 mg per day; efficacy was not systematically assessed above 5 mg per day.[12] Short-term and long-term noncomparative studies demonstrated pergolide's effectiveness in improving motor control and reducing dyskinesia. In a multicenter trial, patients achieved a 5% to 30% reduction in levodopa dosage while sustaining equivalent or improved clinical status, with notable decreases in motor disability scores.[12] Long-term follow-up in open-label studies showed sustained benefits, such as a 42% reduction in mean motor disability scores after 28 months in a cohort of 18 patients, and considerable improvement over baseline in 56% of 41 patients after 2.5 to 3 years.[13][14] Prior to its withdrawal, pergolide was also used off-label for the treatment of hyperprolactinemia and prolactinomas. At doses ranging from 0.025 to 0.5 mg/day, it led to significant tumor shrinkage in over 75% of macroprolactinoma cases.[2] Following its voluntary market withdrawal in 2007 due to risks of cardiac valvulopathy, pergolide is contraindicated for human use in the United States and other regions where it has been removed from availability, limiting its application to historical contexts only.[3] It is contraindicated in patients with known hypersensitivity to the drug or other ergot derivatives.[12]Veterinary Applications
Pergolide is primarily used in veterinary medicine to treat pituitary pars intermedia dysfunction (PPID), also known as equine Cushing's disease, in horses.[15] This condition involves excessive hormone production by the pituitary gland, leading to symptoms such as hypertrichosis (abnormal long hair growth), laminitis (inflammation of the hoof's sensitive tissues), and muscle wasting.[15] By acting as a dopamine agonist, pergolide suppresses the overproduction of adrenocorticotropic hormone (ACTH) from the pituitary, thereby alleviating these clinical signs.[8] The FDA-approved formulation for horses is Prascend (pergolide mesylate) tablets.[9] Treatment typically begins with an oral dose of 0.002 mg/kg (2 mcg/kg) body weight once daily, which can be adjusted based on monitoring of serum ACTH levels to achieve optimal control, not exceeding 0.004 mg/kg daily.[9] Long-term therapy at low doses has demonstrated sustained clinical improvements, including reduced shedding delays and improved coat quality, in 60-80% of treated horses.[16] Since December 1, 2018, pergolide has been granted Therapeutic Use Exemption (TUE) status by the United States Equestrian Federation (USEF) for competition horses diagnosed with PPID, permitting continued administration without a required withdrawal period prior to events.[17] This exemption facilitates ongoing management of the disease in performance animals while ensuring compliance with anti-doping regulations.[17]Pharmacology
Pharmacodynamics
Pergolide is a semisynthetic ergot derivative that functions primarily as a dopamine receptor agonist.[18] It exhibits high affinity for dopamine D2 receptors, where it acts as a full agonist, and demonstrates partial agonism at D1 receptors, with lower affinity compared to D2.[19] [20] Additionally, pergolide shows agonism at several serotonin receptor subtypes, including 5-HT1A (pKi ≈ 8.7), 5-HT2A (pKi ≈ 8.1), 5-HT2B (pKi ≈ 8.2), 5-HT1B (pKi ≈ 6.6), and 5-HT2C (pKi ≈ 6.5), which contribute to its therapeutic effects as well as potential side effects.[19] In terms of potency, pergolide is 10- to 1000-fold more effective than bromocriptine on a milligram-per-milligram basis in suppressing prolactin levels, reflecting its stronger dopaminergic activity.[21] [2] This enhanced potency arises from its robust binding and activation of dopamine receptors, particularly D2 and D3 subtypes (pKi 7.3–9.21 and 8.3–9.07, respectively).[19] Therapeutically, pergolide exerts its effects in Parkinson's disease by directly stimulating postsynaptic dopamine receptors in the nigrostriatal pathway, thereby mimicking endogenous dopamine to improve motor symptoms.[18] This mechanism helps restore dopaminergic signaling in the basal ganglia, addressing the deficits caused by neurodegeneration.[20]Pharmacokinetics
Pergolide is rapidly absorbed following oral administration in humans, achieving peak plasma concentrations within 2-3 hours post-dose.[22] Although exact oral bioavailability remains undetermined due to assay sensitivity limitations, estimates suggest it ranges from 20% to 60%, reflecting significant first-pass hepatic metabolism that produces active metabolites, including pergolide sulfoxide.[23] The elimination half-life of pergolide in humans is approximately 21 hours, with primary renal excretion of metabolites.[22] Protein binding is high, at about 90% to plasma proteins.[22] In horses, pergolide exhibits rapid absorption after oral dosing, with median peak plasma concentrations reached at approximately 0.4 hours following a single 10 mcg/kg dose.[9] The elimination half-life is shorter, averaging 6 hours, and steady-state concentrations are attained within 3 days of daily administration.[24] Protein binding remains around 90%.[9]Adverse Effects
Cardiac Valvulopathy
Pergolide's association with cardiac valvulopathy stems from its potent agonism at the 5-HT2B serotonin receptor, which is expressed on cardiac valve interstitial cells. This receptor activation promotes the transformation of fibroblasts into myofibroblasts, stimulating excessive proliferation and the deposition of extracellular matrix components such as collagen and glycosaminoglycans on valve leaflets. The resulting fibrotic thickening impairs valve coaptation, leading to regurgitation, predominantly affecting the mitral, aortic, and tricuspid valves.[25][26][27] Echocardiographic studies conducted in 2006 and 2007 demonstrated a significantly elevated prevalence of moderate-to-severe valvular regurgitation among long-term pergolide users compared to controls or users of non-ergot dopamine agonists. In a key prevalence study of 155 Parkinson's disease patients, moderate-to-severe regurgitation occurred in 23% of those taking pergolide (versus 0% in the non-ergot group), with similar findings of 29% in cabergoline users highlighting the class effect of ergot-derived agonists. A parallel cohort analysis reported incidence rates of new valvular regurgitation at 30 per 10,000 person-years for pergolide users, conferring a 7-fold increased risk relative to unexposed patients. These abnormalities were often asymptomatic but could progress to require surgical intervention, including valve replacement.[28][29] The risk of valvulopathy proved dose-dependent, with markedly higher incidence at daily doses exceeding 3 mg, where the relative risk escalated to over 37-fold compared to lower doses or non-users. In response, the U.S. Food and Drug Administration mandated baseline and periodic echocardiographic screening for all pergolide users to detect early valvular changes, alongside clinical monitoring for symptoms such as dyspnea, fatigue, or peripheral edema. Doses above 5 mg/day were explicitly discouraged due to amplified fibrotic potential.[29][30] Following pergolide's voluntary market withdrawal in 2007, guidelines emphasized continued cardiac surveillance for former long-term users, particularly those with prior high-dose exposure or echocardiographic evidence of regurgitation at discontinuation. Serial echocardiograms were recommended to assess for regression, as studies observed partial or complete resolution of mild-to-moderate lesions within 1-4 years post-withdrawal, though severe cases may persist and necessitate ongoing follow-up.[31][30]Neurological and Behavioral Effects
Neurological side effects of pergolide, a dopamine agonist used in Parkinson's disease treatment, primarily stem from its stimulation of central dopamine receptors, including D1 and D2 subtypes. Common manifestations include hallucinations, confusion, dyskinesia, and somnolence. In clinical trials, hallucinations occurred in 13.8% of patients receiving pergolide with levodopa, compared to 3.2% on placebo with levodopa, while confusion affected 11.1% versus 9.6%, somnolence 10.1% versus 3.7%, and dyskinesia 62.4% versus 24.6%. These effects, particularly hallucinations and confusion, frequently lead to treatment discontinuation, with hallucinations accounting for 7.8% of such cases. Pergolide is associated with impulse control disorders, such as pathological gambling and hypersexuality, attributable to its dopaminergic activity in mesolimbic pathways. These disorders arise in up to 17% of dopamine agonist users, with a specific incidence of 16% reported for pergolide as an add-on therapy in Parkinson's patients. Such behaviors can significantly impair quality of life and often necessitate dose reduction or drug withdrawal.[32] Orthostatic hypotension and dizziness represent additional frequent neurological adverse effects, especially during initial dosing. Dizziness was reported in 19.1% of pergolide-treated patients versus 13.9% on placebo, and orthostatic hypotension in 9.0% versus 7.0%. These symptoms, linked to peripheral dopamine receptor activation, are typically mitigated through gradual dose titration to minimize autonomic disruption. In elderly Parkinson's patients, long-term pergolide use heightens the risk of persistent confusion, as dopamine agonists like pergolide are more prone to induce or worsen cognitive disturbances compared to levodopa. This vulnerability underscores the need for cautious application in older adults, where such effects may contribute to broader neuropsychiatric decline.Veterinary Adverse Effects
In horses treated for pituitary pars intermedia dysfunction (PPID), pergolide is generally well-tolerated with mild adverse effects, primarily transient anorexia or reduced appetite (affecting up to 20-30% initially), lethargy, and depression, which often resolve within days to weeks with dose adjustment or supportive care. Rare effects include colic, sweating, diarrhea, or mild neurological signs like ataxia. Unlike in humans, no cases of cardiac valvulopathy have been reported in horses as of 2021, based on echocardiographic studies. Hypersensitivity to ergot derivatives is a contraindication. Overdose can lead to more severe signs such as prolonged inappetence or central nervous system depression.[33][34][35]History
Development and Approval
Pergolide, chemically known as (6aR,9R,10aR)-9-(methylsulfanylmethyl)-7-propyl-6,6a,8,9,10,10a-hexahydroindolo[4,3-fg]quinoline, was patented by Eli Lilly and Company in 1978 under U.S. Patent No. 4,166,182 as an ergoline derivative of ergot alkaloids with potent antiparkinsonian activity due to its dopamine agonist properties.[36] The invention described methods for synthesizing 6-n-propyl-8-methoxymethyl or methylmercaptomethylergolines, including pergolide, aimed at addressing dopamine deficiency in Parkinson's disease through direct stimulation of dopamine receptors.[36] The U.S. Food and Drug Administration (FDA) granted approval for pergolide mesylate, marketed as Permax tablets, on December 30, 1988, for adjunctive therapy with levodopa/carbidopa to manage signs and symptoms of idiopathic Parkinson's disease.[37] This approval stemmed from clinical trials demonstrating efficacy in Parkinson's disease.[37] Following U.S. launch, pergolide received marketing authorization in Europe, including the United Kingdom, in 1989, expanding its availability as a dopamine agonist alternative to bromocriptine.[18] By 1990, regulatory approvals for human use had been secured in multiple regions globally, facilitating broader clinical adoption.[18] Throughout the 1990s, pergolide solidified its role as a second-line dopamine agonist for Parkinson's disease, particularly in advanced stages as an adjunct to levodopa, due to its long-acting D1 and D2 receptor agonism allowing once- or twice-daily dosing.[38]Market Withdrawal and Post-Withdrawal Status
In March 2007, the U.S. Food and Drug Administration (FDA) requested the voluntary withdrawal of pergolide from the market for human use, leading manufacturers—including Valeant Pharmaceuticals for the branded product Permax and Par Pharmaceutical and Teva Pharmaceuticals for generics—to discontinue production and distribution due to evidence from echocardiographic studies linking the drug to an increased risk of cardiac valvulopathy.[3][29] These studies, including a 2006 case-control analysis and a 2007 cohort study, demonstrated higher rates of moderate-to-severe valvular regurgitation in pergolide users compared to controls or users of non-ergot dopamine agonists.[39][29] In Europe, the European Medicines Agency (EMA) suspended marketing authorizations for pergolide-containing products for human use in 2007, citing similar concerns over valvular heart disease risks, which prompted a phased global withdrawal for human indications by approximately 2010.[40] Post-withdrawal, availability for human patients became limited to special access programs in select countries, such as compassionate use protocols for refractory Parkinson's disease cases where alternatives are ineffective.[18] As of 2025, no new approvals for human use have been granted in major markets, and routine clinical application remains rare due to the established safety profile.[18] Following the human market withdrawal, pergolide shifted primarily to veterinary applications, particularly for equine pituitary pars intermedia dysfunction (PPID), with widespread use of compounded formulations from 2007 onward under FDA enforcement discretion to address immediate shortages.[41] This discretion ended in March 2012, after the FDA approved Prascend (pergolide mesylate tablets) as the first veterinary-specific product in September 2011, standardizing dosing and quality control for animal use.[42][41]Society and Culture
Brand Names
Pergolide has been marketed under several brand names for human and veterinary use, though human formulations were largely discontinued following safety concerns related to cardiac valvulopathy.[3] For human use, the primary brand was Permax, produced by Eli Lilly and Company, which was available in tablet form until its voluntary withdrawal from the U.S. market in 2007 along with generic pergolide mesylate equivalents.[3] Internationally, Celance, also by Eli Lilly, was marketed in regions including Argentina, Brazil, Chile, China, and several others in Latin America, Asia, and Europe (e.g., England, France, Ireland), but it has since been discontinued in line with global restrictions on human pergolide products.[2] As of 2025, no active proprietary or generic brands of pergolide remain available for human use worldwide. In veterinary medicine, particularly for treating pituitary pars intermedia dysfunction (PPID) in horses, Prascend tablets (pergolide mesylate) by Boehringer Ingelheim received FDA approval in 2011 and continues to be the leading brand in the United States and other markets.[43] In Europe and select international regions, Pergoquin tablets (1 mg pergolide) by Ceva Santé Animale serve as a comparable proprietary option for equine PPID management.[44] Additionally, Pergocoat tablets (0.5 mg and 1 mg pergolide) by Dechra, launched in 2024, is available for equine PPID treatment in the United Kingdom and Europe.[45] Following the human market withdrawal, compounded pergolide formulations were temporarily permitted for veterinary use from 2007 to 2012 until approved brands like Prascend became available, after which compounding was phased out by FDA directive.[41]| Brand Name | Type | Manufacturer | Status (as of 2025) | Primary Regions |
|---|---|---|---|---|
| Permax | Human | Eli Lilly | Discontinued (2007) | United States |
| Celance | Human | Eli Lilly | Discontinued | Latin America, Asia, Europe |
| Prascend | Veterinary | Boehringer Ingelheim | Active | United States, Global |
| Pergoquin | Veterinary | Ceva Santé Animale | Active | Europe |
| Pergocoat | Veterinary | Dechra | Active | United Kingdom, Europe |