Pharmacokinetics and Comparative Bioavailability of Apomorphine Sublingual Film and Subcutaneous Apomorphine Formulations in Patients with Parkinson’s Disease and “OFF” Episodes: Results of a Randomized, Three-Way Crossover, Open-Label Study

Agbo, Felix; Isaacson, Stuart; Gil, Ramon; Chiu, Yu-Yuan; Brantley, Scott J.; Bhargava, Parul; Navia, Bradford

doi:10.1007/s40120-021-00251-6

Cited by 20 publications

(33 citation statements)

References 22 publications

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“…18 Importantly in the current study, QT prolongation was not observed at apomorphine C max , despite administration of apomorphine sublingual film doses exceeding those needed to achieve FULL "ON," perhaps owing to the slower rate of absorption of sublingual versus subcutaneous apomorphine. 18 There was a nonlinear relationship between C max and dose, likely due to high interpatient variability. This relationship may have also been influenced by route of administration, which requires adequate moisture in the oral cavity to facilitate dissolution of the sublingual film.…”

Section: Discussioncontrasting

confidence: 49%

“…In a pharmacokinetic comparative bioavailability study, apomorphine sublingual film had a lower C max compared with subcutaneous apomorphine formulations at similar exposures 18 . Importantly in the current study, QT prolongation was not observed at apomorphine C max , despite administration of apomorphine sublingual film doses exceeding those needed to achieve FULL “ON,” perhaps owing to the slower rate of absorption of sublingual versus subcutaneous apomorphine 18 . There was a nonlinear relationship between C max and dose, likely due to high interpatient variability.…”

Section: Discussionmentioning

confidence: 99%

“…17 A prior study found that maximum plasma concentration (C max ) was lower and time to C max (T max ) was longer for apomorphine sublingual film compared with subcutaneous apomorphine formulations, while overall systemic apomorphine exposure was similar. 18 The pharmacokinetic properties of apomorphine sublingual film may contribute to a more favorable safety profile than other apomorphine formulations, as similar overall exposure is achieved without a rapid early rise in drug concentration. In a pivotal study, apomorphine sublingual film demonstrated a significant improvement in the Movement Disorder Society Unified Parkinson's Disease Rating Scale Part III motor examination score at 30 minutes postdose compared with placebo (least squares [LS] mean difference -7.6, P = 0.0002).…”

mentioning

confidence: 99%

“…Apomorphine sublingual film, a novel sublingual formulation of apomorphine, is approved for the acute, intermittent treatment of “OFF” episodes associated with PD 17 . A prior study found that maximum plasma concentration (C max ) was lower and time to C max (T max ) was longer for apomorphine sublingual film compared with subcutaneous apomorphine formulations, while overall systemic apomorphine exposure was similar 18 . The pharmacokinetic properties of apomorphine sublingual film may contribute to a more favorable safety profile than other apomorphine formulations, as similar overall exposure is achieved without a rapid early rise in drug concentration.…”

mentioning

confidence: 99%

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A Randomized Thorough QT Study of Apomorphine Sublingual Film in Patients With Parkinson's Disease

Stocchi

Peckham

Pandis

et al. 2022

Clinical Pharm in Drug Dev

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A randomized thorough QT study was conducted to assess the effects of apomorphine sublingual film (SL-APO) on corrected QT interval (QTc) and other cardiac conduction parameters in patients with Parkinson's disease (PD) and "OFF" episodes. Patients were titrated to an SL-APO dose that resulted in FULL "ON," followed by up to two additional doses (maximum 60 mg), then randomized at the highest tolerated dose to a treatment sequence of SL-APO, placebo, and moxifloxacin (400 mg, positive control) in a three-way crossover design. Changes from baseline in time-matched, placeboadjusted Fridericia-corrected QTc interval ( QTcF) and Bazett-corrected QTc interval ( QTcB) were analyzed from postdose electrocardiograms. Forty patients were randomized and received single doses of study treatments. Upper limits of 90% confidence intervals (CIs) for QTcF of SL-APO were below the 10-millisecond regulatory threshold at all prespecified timepoints, demonstrating no clinically significant effect on QTcF. Lower limits of 90% CIs for QTcF of moxifloxacin exceeded the 5-millisecond regulatory threshold at all timepoints up to 3 hours, confirming assay sensitivity.SL-APO had no clinically meaningful effects on QTcB,PR/QRS intervals,heart rate,or electrocardiogramderived morphology (EudraCT identifier: 2016-001762-29; ClinicalTrials.gov identifier: NCT03187301).

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Section: Discussioncontrasting

confidence: 49%

Section: Discussionmentioning

confidence: 99%

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confidence: 99%

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confidence: 99%

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A Randomized Thorough QT Study of Apomorphine Sublingual Film in Patients With Parkinson's Disease

Stocchi

Peckham

Pandis

et al. 2022

Clinical Pharm in Drug Dev

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“…There have been attempts to develop alternate modes of administration, but to date, all have failed primarily due to subcutaneous tissue side effects. APL-130277 is a new formulation of apomorphine that consists of a sublingual, bilayer film formulation, first registered in Canada in 2020 and FDA approved as treatment for unpredictable OFF episodes [ 96 , 97 ]. A 12-week, Phase 3, DBRCT involving patients with OFF episodes despite stable anti-PD treatment evaluated sublingual apomorphine (dose range of 10–30 mg) and reported significantly greater self-rated full ON response within 30 min versus placebo, corroborated by a nominally significant full ON response using home-dosing diaries.…”

Section: Motor Fluctuationsmentioning

confidence: 99%

Newly Approved and Investigational Drugs for Motor Symptom Control in Parkinson's Disease

Luca

Reyes

Fox

2022

Drugs

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Motor symptoms are a core feature of Parkinson’s disease (PD) and cause a significant burden on patients’ quality of life. Oral levodopa is still the most effective treatment, however, the motor benefits are countered by inherent pharmacologic limitations of the drug. Additionally, with disease progression, chronic levodopa leads to the appearance of motor complications including motor fluctuations and dyskinesia. Furthermore, several motor abnormalities of posture, balance, and gait may become less responsive to levodopa. With these unmet needs and our evolving understanding of the neuroanatomic and pathophysiologic underpinnings of PD, several advances have been made in defining new therapies for motor symptoms. These include newer levodopa formulations and drug delivery systems, refinements in adjunctive medications, and non-dopaminergic treatment strategies. Although some are in early stages of development, these novel treatments potentially widen the available options for the management of motor symptoms allowing clinicians to provide an individually tailored care for PD patients. Here, we review the existing and emerging interventions for PD with focus on newly approved and investigational drugs for motor symptoms, motor fluctuations, dyskinesia, and balance and gait dysfunction.

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Alzheimer's and Parkinson's disease therapies in the clinic

Chopade

Zhao

et al. 2022

Bioengineering & Transla Med

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Alzheimer's disease (AD) and Parkinson's disease (PD) are the most prevalent neurodegenerative diseases, affecting millions and costing billions each year in the United States alone. Despite tremendous progress in developing therapeutics that manage the symptoms of these two diseases, the scientific community has yet to develop a treatment that effectively slows down, inhibits, or cures neurodegeneration. To gain a better understanding of the current therapeutic frontier for the treatment of AD and PD, we provide a review on past and present therapeutic strategies for these two major neurodegenerative disorders in the clinical trial process. We briefly recap currently US Food and Drug Administration‐approved therapies, and then explore trends in clinical trials across the variables of therapy mechanism of disease intervention, administration route, use of delivery vehicle, and outcome measures, across the clinical phases over time for “Drug” and “Biologic” therapeutics. We then present the success rate of past clinical trials and analyze the intersections in therapeutic approaches for AD and PD, revealing the shift in clinical trials away from therapies targeting neurotransmitter systems that provide symptomatic relief, and towards anti‐aggregation, anti‐inflammatory, anti‐oxidant, and regeneration strategies that aim to inhibit the root causes of disease progression. We also highlight the evolving distribution of the types of “Biologic” therapies investigated, and the slowly increasing yet still severe under‐utilization of delivery vehicles for AD and PD therapeutics. We then briefly discuss novel preclinical strategies for treating AD and PD. Overall, this review aims to provide a succinct overview of the clinical landscape of AD and PD therapies to better understand the field's therapeutic strategy in the past and the field's evolution in approach to the present, to better inform how to effectively treat AD and PD in the future.

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Pharmacokinetics and Comparative Bioavailability of Apomorphine Sublingual Film and Subcutaneous Apomorphine Formulations in Patients with Parkinson’s Disease and “OFF” Episodes: Results of a Randomized, Three-Way Crossover, Open-Label Study

Cited by 20 publications

References 22 publications

A Randomized Thorough QT Study of Apomorphine Sublingual Film in Patients With Parkinson's Disease

A Randomized Thorough QT Study of Apomorphine Sublingual Film in Patients With Parkinson's Disease

Newly Approved and Investigational Drugs for Motor Symptom Control in Parkinson's Disease

Alzheimer's and Parkinson's disease therapies in the clinic

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