Dopamine D2R Agonist-Induced Cardiovascular Effects in Healthy Male Subjects: Potential Implications in Clinical Settings

Farha, Khalid Abou; Baljé-Volkers, Corine; Tamminga, Wim J.; Daas, Izaak den; Os, Sandra van

doi:10.1155/2014/956353

Cited by 11 publications

(11 citation statements)

References 39 publications

(51 reference statements)

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“…In human, dopamine D2 receptor agonist can cause adverse cardiovascular morbidity. [31][32][33] Histidine is an essential amino acid. In a study among 1,898 female participants, although not significant, higher dietary intake of histidine resulted in lower PWV.…”

Section: Discussionmentioning

confidence: 99%

Novel Metabolites Are Associated With Augmentation Index and Pulse Wave Velocity: Findings From the Bogalusa Heart Study

et al. 2019

American Journal of Hypertension

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Arterial stiffness measured by aortic pulse wave velocity (PWV) and augmentation index (AI) is a marker of subclinical organ damage and an independent risk factor for cardiovascular disease events and mortality. 1-5 Although many factors, including aging, diabetes, hypertension, dyslipidemia, and chronic kidney disease, contribute to arterial stiffening, the pathophysiological mechanisms of this process are still not fully understood. Circulating low-weight metabolites represent the intermediate and end products of metabolic pathways and may reflect initial stages of arterial stiffness. Recent advances in metabolomics technology have allowed for global characterization of a large panel of metabolites from biological samples, which provides a unique opportunity for investigating arterial stiffness mechanisms. Previous metabolomics studies have identified important metabolites associated with arterial stiffness, 6-8 revealing novel mechanisms of arterial stiffening. 6-8 However, these studies either had small sample sizes or only assayed a limited number of metabolites, and omitted metabolite networks. In this study, we performed untargeted metabolomics profiling using the most up-to-date metabolites panel in 1,239 participants of the Bogalusa Heart Study (BHS) to identify

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Section: Discussionmentioning

confidence: 99%

Novel Metabolites Are Associated With Augmentation Index and Pulse Wave Velocity: Findings From the Bogalusa Heart Study

et al. 2019

American Journal of Hypertension

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“…Moreover, authors suggest that nonphysiological increased chronic pulsatile stress (equal to pulse pressure * heart rate) may result in endothelial cell dysfunction through a variety of pathophysiological mechanisms. [33][34][35] Our findings that men and older individuals treated with pramipexole were more likely than those not receiving pramipexole to be diagnosed with HF have several possible explanations. HF is more prevalent in men than women at all ages, even after adjusting for common HF risk factors, such as obesity and diabetes.…”

Section: Discussionmentioning

confidence: 97%

“…Statistically significant increases in mean systolic blood pressure, heart rate, pulse pressure, and resting pulse pressure were observed in a dose‐dependent fashion. Moreover, authors suggest that nonphysiological increased chronic pulsatile stress (equal to pulse pressure * heart rate) may result in endothelial cell dysfunction through a variety of pathophysiological mechanisms …”

Section: Discussionmentioning

confidence: 99%

“…Although biological mechanisms by which pramipexole could potentially cause HF remain unclear, a recent phase I clinical trial suggests that drug-induced supraphysiologic increases in vital signs underlie the associations between D2 receptor agonists and HF. 33 In this trial, pramipexole was administered to 52 healthy male subjects in escalating doses over 13 days and serial measurements of blood pressure and heart rate were analyzed. Statistically significant increases in mean systolic blood pressure, heart rate, pulse pressure, and resting pulse pressure were observed in a dose-dependent fashion.…”

Section: Discussionmentioning

confidence: 99%

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Associations Between Cardiovascular Events and Nonergot Dopamine Agonists in Parkinson's Disease

Crispo

Willis

Thibault

et al. 2015

Movement Disord Clin Pract

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Background Knowledge of possible cardiovascular risks from Parkinson's disease (PD) medications is critical to informing safe and effective treatment decisions. The objective of our study was to determine whether PD patients treated with nonergot dopamine agonists (DAs) are at increased risk of adverse cardiovascular or cerebrovascular outcomes, relative to PD patients receiving other treatments. Methods Matched case‐control studies were conducted within a cohort of 14,122 inpatients receiving treatment for PD who were identified in the Cerner Health Facts database. Primary outcomes were associations between nonergot DA use and diagnosis of adverse cardiovascular events (acute myocardial infarction, heart failure [HF], hypotension, and valvulopathy). Secondary outcomes included associations between nonergot DA use and diagnosis of adverse cerebrovascular events (cerebrovascular accident and ischemic stroke) and odds of significant exposure‐outcome relationships by patient factors. Results HF was the only adverse event that demonstrated a significant association with nonergot DA use. Individuals treated with pramipexole were more likely to be diagnosed with HF, relative to no use (adjusted odds ratio [AOR]: 1.28; 95% confidence interval [CI]: 1.07–1.53). The association between pramipexole and HF was greater among individuals treated with pramipexole monotherapy (relative to levodopa monotherapy) (AOR, 1.50; 95% CI: 1.09–2.06). Compared to nonusers, men and older individuals treated with pramipexole were more likely to be diagnosed with HF. Conclusions Results from our study suggest an association between pramipexole use and HF. Findings warrant replication; however, individuals with PD and independent risk factors for, or a history of, HF may benefit from limited use of this drug.

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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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Dopamine D2R Agonist-Induced Cardiovascular Effects in Healthy Male Subjects: Potential Implications in Clinical Settings

Cited by 11 publications

References 39 publications

Novel Metabolites Are Associated With Augmentation Index and Pulse Wave Velocity: Findings From the Bogalusa Heart Study

Novel Metabolites Are Associated With Augmentation Index and Pulse Wave Velocity: Findings From the Bogalusa Heart Study

Associations Between Cardiovascular Events and Nonergot Dopamine Agonists in Parkinson's Disease

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

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