Comparison of pramipexole with and without domperidone co‐administration on alertness, autonomic, and endocrine functions in healthy volunteers

Samuels, E. R.; Hou, Ruihua; Langley, R. W.; Szabadi, E.; Bradshaw, C. M.

doi:10.1111/j.1365-2125.2007.02938.x

Cited by 19 publications

(18 citation statements)

References 52 publications

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“…Although pramipexole is a non-ergot D 2 / D 3 agonist (and is clinically used as such in Parkinson’s disease, restless leg syndrome, and occasionally in treatment-resistant MDD), it has previously been found to have behavioural effects of a DA antagonist at the low doses (0.5 mg) used in our dataset [72-74]. Similarly, low doses of the D 2 agonist cabergoline have been found to specifically reduce reward go learning [75].…”

Section: Discussionmentioning

confidence: 99%

Mapping anhedonia onto reinforcement learning: a behavioural meta-analysis

Huys

Pizzagalli

Bogdan

et al. 2013

Biol Mood Anxiety Disord

426

361

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BackgroundDepression is characterised partly by blunted reactions to reward. However, tasks probing this deficiency have not distinguished insensitivity to reward from insensitivity to the prediction errors for reward that determine learning and are putatively reported by the phasic activity of dopamine neurons. We attempted to disentangle these factors with respect to anhedonia in the context of stress, Major Depressive Disorder (MDD), Bipolar Disorder (BPD) and a dopaminergic challenge.MethodsSix behavioural datasets involving 392 experimental sessions were subjected to a model-based, Bayesian meta-analysis. Participants across all six studies performed a probabilistic reward task that used an asymmetric reinforcement schedule to assess reward learning. Healthy controls were tested under baseline conditions, stress or after receiving the dopamine D2 agonist pramipexole. In addition, participants with current or past MDD or BPD were evaluated. Reinforcement learning models isolated the contributions of variation in reward sensitivity and learning rate.ResultsMDD and anhedonia reduced reward sensitivity more than they affected the learning rate, while a low dose of the dopamine D2 agonist pramipexole showed the opposite pattern. Stress led to a pattern consistent with a mixed effect on reward sensitivity and learning rate.ConclusionReward-related learning reflected at least two partially separable contributions. The first related to phasic prediction error signalling, and was preferentially modulated by a low dose of the dopamine agonist pramipexole. The second related directly to reward sensitivity, and was preferentially reduced in MDD and anhedonia. Stress altered both components. Collectively, these findings highlight the contribution of model-based reinforcement learning meta-analysis for dissecting anhedonic behavior.

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Section: Discussionmentioning

confidence: 99%

Mapping anhedonia onto reinforcement learning: a behavioural meta-analysis

Huys

Pizzagalli

Bogdan

et al. 2013

Biol Mood Anxiety Disord

426

361

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“…Further, ABT-925 showed significant effect on executive function and emotion recognition in the same sample (Gross et al, 2013). Most of the evidence is derived from the effects of preferential D 3 receptor-agonists, pramipexole (5- to 7-fold D 3 /D 2 and D 4 receptor selectivity) (Brusa et al, 2003; Hubble, 2000; Rektorova et al, 2005; Samuels et al, 2006a, b, 2007) and rotigotine (20-fold D 3 /D 2 and 100-fold D 3 /D 1 receptor selectivity) (Bunten and Happe, 2006; Sanford and Scott, 2011; Scheller et al, 2009) on cognition in healthy individuals and those with PD or bipolar disorder. Thus far, the cognitive effects of preferential D 3 receptor agonists in humans are mixed (Brusa et al, 2005).…”

Section: Pharmacological Dopamine D3 Receptor Intervention and Cogmentioning

confidence: 99%

The potential role of dopamine D3 receptor neurotransmission in cognition

Nakajima¹,

Gerretsen²,

Takeuchi³

et al. 2013

European Neuropsychopharmacology

161

120

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Currently available treatments have limited pro-cognitive effects for neuropsychiatric disorders, such as schizophrenia, Parkinson’s disease and Alzheimer’s disease. The primary objective of this work is to review the literature on the role of dopamine D3 receptors in cognition, and propose dopamine D3 receptor antagonists as possible cognitive enhancers for neuropsychiatric disorders. A literature search was performed to identify animal and human studies on D3 receptors and cognition using PubMed, MEDLINE and EMBASE. The search terms included “dopamine D3 receptor” and “cognition”. The literature search identified 164 articles. The results revealed: (1) D3 receptors are associated with cognitive functioning in both healthy individuals and those with neuropsychiatric disorders; (2) D3 receptor blockade appears to enhance while D3 receptor agonism seems to impair cognitive function, including memory, attention, learning, processing speed, social recognition and executive function independent of age; and (3) D3 receptor antagonists may exert their pro-cognitive effect by enhancing the release of acetylcholine in the prefrontal cortex, disinhibiting the activity of dopamine neurons projecting to the nucleus accumbens or prefrontal cortex, or activating CREB signaling in the hippocampus. These findings suggest that D3 receptor blockade may enhance cognitive performance in healthy individuals and treat cognitive dysfunction in individuals with a neuropsychiatric disorder. Clinical trials are needed to confirm these effects.

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“…III score was tested in order to meet the FDA's criteria for the approval of pramipexole ER in the USA [30]. [16,18,21] Lacks affinity for receptors of the dopamine D 1 subfamily a [22] Lacks affinity for a 1 -adrenergic, b-adrenergic, ACh, and serotonin 5-HT 1A and 5-HT 2 receptors [22] Demonstrated dopaminergic activity in animal models of PD [13,23] Demonstrated numerous potential neuroprotective actions in preclinical models of PD [24] ; Dopamine neuronal degeneration in pts with early PD c [25] ; Prolactin and : growth hormone levels in healthy volunteers [26] No effect on QT interval in healthy volunteers [27] Up-titration of PPX ER at faster than the recommended rate : BP and : HR in healthy volunteers d [8,10,28] Up-titration of PPX ER at the recommended rate did not : BP and : HR in pts with PD [8,10] Up-titration of PPX ER at the recommended rate occasionally caused symptomatic orthostatic hypotension in pts with PD e [10] ACh acetylcholine, BP blood pressure, HR heart rate, L-DOPA levodopa, PD Parkinson's disease, PL placebo, PPX ER pramipexole extended release, pts patients, ; decreased, : increased a D 1 subfamily includes D 1 and D 5 receptors; D 2 subfamily includes D 2 , D 3 and D 4 receptors b Binding affinity (K i ) of 3.9, 3.3, 0.5 and 3.9 nmol/L at D 2L , D 2S , D 3 and D 4 receptor subtypes, respectively [21] c p = 0.01 vs. L-DOPA; as assessed by dopamine transporter brain imaging d Albeit mean values remained within normal reference ranges e Reported in 3 % of pts with early or advanced PD who received PPX ER in two large PL-controlled trials [10] (see Sect. 4.2.2) Monotherapy with pramipexole ER administered once daily was noninferior to monotherapy with pramipexole IR administered three times daily and significantly more effective than placebo in improving activities of daily living and motor function in patients with early PD [11].…”

Section: Patients With Early Parkinson's Diseasementioning

confidence: 99%

Pramipexole Extended-Release: A Review of Its Use in Patients with Parkinson’s Disease

Frampton

2014

Drugs

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Pramipexole, a non-ergolinic, D3-preferring dopamine agonist (DA), is well established as a treatment option for motor symptoms at all stages of Parkinson's disease (PD). It is administered orally and is available as both a three-times daily immediate-release (IR) formulation and a once-daily extended-release (ER) formulation (Mirapex(®) ER, Mirapexin(®) ER; Pexola(®) ER, Sifrol(®) ER). The two formulations are bioequivalent; the majority (>80 %) of patients can be switched overnight from pramipexole IR to ER without the need for dosage adjustment. In terms of improving activities of daily living and motor function in short-term (≤33-week), double-blind studies, pramipexole ER was noninferior to pramipexole IR and significantly more effective than placebo as monotherapy in patients with early PD, and similar to pramipexole IR and significantly more effective than placebo as adjunctive therapy to levodopa in patients with advanced PD. In long-term (80-week) extensions of these trials, open-label treatment with pramipexole ER was associated with sustained symptomatic benefit. Moreover, the majority of extension participants who responded to a simple convenience questionnaire expressed a preference for once-daily over three-times daily dosing. Pramipexole ER was generally well tolerated in clinical trials; no new or unexpected safety signals were identified compared with the IR formulation. Head-to-head trials are needed in order to fully define the role of pramipexole ER relative to other once-daily formulations of DAs (oral ropinirole and transdermal rotigotine). Nonetheless, by reducing the pill burden, the ER formulation of pramipexole provides a more convenient alternative to the IR formulation; studies specifically testing whether this translates into improved patient compliance and symptom control are worthwhile.

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Comparison of pramipexole with and without domperidone co‐administration on alertness, autonomic, and endocrine functions in healthy volunteers

Cited by 19 publications

References 52 publications

Mapping anhedonia onto reinforcement learning: a behavioural meta-analysis

Mapping anhedonia onto reinforcement learning: a behavioural meta-analysis

The potential role of dopamine D3 receptor neurotransmission in cognition

Pramipexole Extended-Release: A Review of Its Use in Patients with Parkinson’s Disease

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