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Pharmacokinetics of Opicapone and Effect on COMT and Levodopa Pharmacokinetics in Patients with Parkinson’s Disease

G. Loewen, P. Lewitt, C. Olanow, K. Kieburtz, G. Liang, R. Jimenez, K. Olson, E. Roberts (San Diego, CA, USA)

Meeting: 2019 International Congress

Abstract Number: 143

Keywords:

Session Information

Date: Monday, September 23, 2019

Session Title: Clinical Trials, Pharmacology and Treatment

Session Time: 1:45pm-3:15pm

Location: Agora 3 West, Level 3

Objective: To evaluate the pharmacokinetics and pharmacodynamics of opicapone in Parkinson’s disease (PD).

Background: Opicapone, a highly selective COMT inhibitor, is approved in Europe and under development in the U.S. as an adjunct to levodopa in adults with PD and motor fluctuation.

Method: Patients with stable PD were administered once-daily opicapone (50 mg) in the evening on Days 1-14. Serial blood samples for determination of plasma opicapone concentrations and erythrocyte soluble COMT (S-COMT) activity were collected after the first and last opicapone dose. Participants were randomized to receive carbidopa/levodopa (25/100 mg) every 3 or 4 hours (Q3H or Q4H) on pharmacokinetic sampling days, and their usual carbidopa/levodopa regimen on other days. Serial plasma samples for determination of levodopa and 3-O-methyldopa concentrations were collected after the first three levodopa doses on Day 1 (prior to opicapone dosing), Day 2 and Day 15. The effect of opicapone on levodopa pharmacokinetics and S-COMT activity was assessed. Mean values (±standard deviations) are presented.

Results: The study enrolled 16 participants (men=10, women=6). Day 14 opicapone Cmax and AUC0-last were 459±252 ng/mL and 2022±783 ng/mL*hr, respectively. At steady-state (Day 14), COMT activity was inhibited on average by 76.3±5.4%, compared to baseline. After opicapone administration, total levodopa AUC (ng/mL*hr) increased from Day 1 (Q3H, 7339±2512; Q4H, 7570±2675) to Day 15 (Q3H, 11714±4429; Q4H, 13159±4528). Peak-to-trough fluctuation in levodopa concentrations for the third daily levodopa dose were reduced from 88.3±40.3% and 173±51.9% for the Q3H and Q4H regimens on Day 1 to 58.1±23.0% and 94.3±25.9%, respectively, on Day 15. Trough levodopa concentrations for the third daily levodopa dose increased from 547±134 and 227±80 ng/mL for the Q3H and Q4H regimens on Day 1 to 1142±532 and 749±354 ng/mL, respectively, on Day 15.

Conclusion: Once-daily opicapone 50 mg resulted in substantial and prolonged COMT inhibition, which increased systemic exposure to levodopa and led to both decreased peak-to-trough fluctuations in levodopa concentrations and to higher trough levodopa concentrations.

To cite this abstract in AMA style:

G. Loewen, P. Lewitt, C. Olanow, K. Kieburtz, G. Liang, R. Jimenez, K. Olson, E. Roberts. Pharmacokinetics of Opicapone and Effect on COMT and Levodopa Pharmacokinetics in Patients with Parkinson’s Disease [abstract]. Mov Disord. 2019; 34 (suppl 2). https://www.mdsabstracts.org/abstract/pharmacokinetics-of-opicapone-and-effect-on-comt-and-levodopa-pharmacokinetics-in-patients-with-parkinsons-disease/. Accessed November 21, 2024.

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