Rotigotine transdermal system as add-on to oral dopamine agonist in advanced Parkinson's disease: An open-label study
Journal
BMC Neurology
Journal Volume
15
Journal Issue
1
Pages
17
Date Issued
2015
Author(s)
Kim J.-M
Chung S.J
Kim J.W
Jeon B.S
Singh P
Thierfelder S
Ikeda J
Bauer L
Sohn Y.-H
Lee M.S
Kim S.J
Cho J.W
Kim H.T
Park K.W
Lee H.-W
Irene L
Abd Aziz Z.B
Sim S.H
Tsai C.-H
Zheng T.-J
Schwartz R
Beran R
Evans A
Hayes M
Tan L
Tan E.K
Asia Pacific Rotigotine Add-on Study Group
Abstract
Background: Achieving optimal symptom control with minimal side effects is a major goal in clinical practice. Dual-agent dopamine receptor agonist (DA) therapy in Parkinson's disease (PD) may represent a promising approach to treatment, as the combination of different pharmacokinetic/pharmacological profiles may result in a lesser need for high dosages and, accordingly, may be well tolerated. The objective of the current study was to investigate safety and efficacy of rotigotine transdermal system as add-on to oral DA in patients with advanced PD inadequately controlled with levodopa and low-dose oral DA. Methods: PD0015 was an open-label, multinational study in patients with advanced-PD and sleep disturbance or early-morning motor impairment. Patients were titrated to optimal dose rotigotine (? 8 mg/24 h) over 1-4 weeks and maintained for 4-7 weeks (8-week treatment). Dosage of levodopa and oral DA (pramipexole ? 1.5 mg/day, ropinirole ? 6.0 mg/day) was stable. Primary variable was Clinical Global Impressions (CGI) item 4: side effects, assessing safety. Other variables included adverse events (AEs), Patient Global Impressions of Change (PGIC), Unified Parkinson's Disease Rating Scale (UPDRS) II and III, Parkinson's Disease Sleep Scale (PDSS-2), Pittsburgh Sleep Quality Index (PSQI), and "off" time. Results: Of 90 patients who received rotigotine, 79 (88%) completed the study; 5 (6%) withdrew due to AEs. Most (83/89; 93%) had a CGI-4 score < 3 indicating that rotigotine add-on therapy did not interfere with functioning; 6 (7%) experienced drug-related AEs that interfered with functioning (score ? 3). AEs occurring in ? 5% were application site pruritus (13%), dizziness (10%), orthostatic hypotension (10%), nausea (8%), dyskinesia (8%), and nasopharyngitis (6%). Numerical improvements in motor function (UPDRS III), activities of daily living (UPDRS II), sleep disturbances (PDSS-2, PSQI), and reduction in "off" time were observed. The majority (71/88; 81%) improved on PGIC. Conclusions: Addition of rotigotine transdermal system to low-dose oral DA in patients with advanced-PD was feasible and may be associated with clinical benefit. ? 2015 Kim et al.
Subjects
Advanced Parkinson's disease; Dual therapy; Oral dopamine receptor agonist; Rotigotine transdermal system; Safety
SDGs
Other Subjects
pramipexole; ropinirole; rotigotine; benzothiazole derivative; dopamine receptor stimulating agent; indole derivative; levodopa; pramipexole; ropinirole; rotigotine; tetralin derivative; thiophene derivative; add on therapy; adult; aged; application site pruritus; Article; Clinical Global Impression scale; daily life activity; dizziness; dose response; drug dose titration; drug efficacy; drug exposure; drug safety; drug tolerability; drug withdrawal; dyskinesia; female; hallucination; human; hyperhidrosis; insomnia; low drug dose; major clinical study; male; motor dysfunction; multicenter study; nausea; orthostatic hypotension; Parkinson disease; phase 3 clinical trial; Pittsburgh Sleep Quality Index; rash; rhinopharyngitis; treatment duration; clinical trial; cutaneous drug administration; middle aged; Parkinson disease; Sleep Wake Disorders; Activities of Daily Living; Administration, Cutaneous; Aged; Benzothiazoles; Dopamine Agonists; Female; Humans; Indoles; Levodopa; Male; Middle Aged; Parkinson Disease; Sleep Wake Disorders; Tetrahydronaphthalenes; Thiophenes
Type
journal article