Clinical Evaluation of Ropinirole PR/XR Tablets in Monotherapy for Parkinson's Disease (PD)

August 30, 2018 updated by: GlaxoSmithKline

Clinical Evaluation of Ropinirole PR/XR Tablets in Monotherapy for Parkinson's Disease - an Open-Label, Uncontrolled Study -

This study was designed to evaluate the pharmacokinetic profile, safety and efficacy in Parkinson's Disease patients.

Study Overview

Status

Completed

Conditions

Intervention / Treatment

Study Type

Interventional

Enrollment (Actual)

62

Phase

  • Phase 2

Contacts and Locations

This section provides the contact details for those conducting the study, and information on where this study is being conducted.

Study Locations

  • Japan
      • Aichi, Japan, 455-8530
        • GSK Investigational Site
      • Aichi, Japan, 460-0008
        • GSK Investigational Site
      • Chiba, Japan, 279-0021
        • GSK Investigational Site
      • Ehime, Japan, 791-0295
        • GSK Investigational Site
      • Hokkaido, Japan, 070-0901
        • GSK Investigational Site
      • Iwate, Japan, 020-0878
        • GSK Investigational Site
      • Kanagawa, Japan, 251-0038
        • GSK Investigational Site
      • Kyoto, Japan, 600-8811
        • GSK Investigational Site
      • Osaka, Japan, 570-8507
        • GSK Investigational Site
      • Saitama, Japan, 343-0032
        • GSK Investigational Site
      • Tokyo, Japan, 113-8431
        • GSK Investigational Site
      • Tokyo, Japan, 136-0075
        • GSK Investigational Site

Participation Criteria

Researchers look for people who fit a certain description, called eligibility criteria. Some examples of these criteria are a person's general health condition or prior treatments.

Eligibility Criteria

Ages Eligible for Study

20 years and older (Adult, Older Adult)

Accepts Healthy Volunteers

No

Genders Eligible for Study

All

Description

Inclusion Criteria:

  • Patients who are diagnosed with PD with severity of the Modified Hoehn & Yahr staging at Stage I to III.
  • Age: 20 years or older (at the time of giving informed consent)
  • Gender: male and female
  • Both inpatient and outpatient status
  • Informed consent: Patients who are able to give informed written consent in person (i.e. patients who are capable of giving informed written consent on one's own)
  • Limited prior exposure to low or moderate doses of L-dopa (up to 3 months in total) or dopamine agonists (up to 6 months in total) provided treatment is discontinued for a minimum of 4 weeks prior to screening.

Exclusion Criteria:

  • Patients who present serious physical signs and symptoms other than those of the PD (e.g. cardiac/hepatic/renal disorder and haematopoietic disorder). The seriousness refers to Grade 3 according to "the Classification of the Severity of Adverse Experiences (Pharmaceutical affairs bureau/Safety division (PAB/SD) Notification No. 80, dated 29 June 1992).
  • Patients with symptomatic postural hypotension. (e.g. dizziness and syncope).
  • Patients who have had serious psychiatric symptoms (e.g. confusion, hallucination, delusion, abnormal behaviour, alcohol or drug dependence) during the past six months (26 weeks) (including symptoms caused by anti-Parkinson drugs).

  • Patients who have been treated with the following drugs at Week -4, and whose treatment regimen of the drug has been changed from Week -4 to Week 0.

    • Anticholinergic agents: trihexyphenidyl hydrochloride (e.g. Artane®), piroheptine hydrochloride (Trimol®), mazaticol hydrochloride (Pentona®), metixene hydrochloride (Cholinfall®), biperiden hydrochloride (Akineton®), profenamine (Parkin®)
    • amantadine hydrochloride (e.g. Symmetrel®)
    • droxidopa (Dops®)
    • citicoline (e.g. Nicholin®)
    • selegiline hydrochloride (FP®)
    • zonisamide
    • estrogen: estriol (e.g.Estriel®)
    • CYP1A2 inhibitors: Ciprofloxacin HCl (e.g. Ciproxan®, enoxacin and fluvoxamine)
  • Patients with severe dementia such as score 3 or 4 of the UPDRS Part I (Mentation, behaviour, and mood)
  • Female patients who are pregnant or lactating, who may be pregnant, or who plan for pregnancy during the study or within 30 days after the last dose of the study drug.
  • Patients with current history or complication of carcinoma or malignant tumour.
  • Patients who have history of drug allergy to ropinirole hydrochloride (HCl).
  • Patients who have received surgical treatment for PD in the past (e.g. pallidectomy, deep brain stimulation).
  • Patients who have been treated with any other investigational drug within 12weeks prior to the treatment phase.
  • Others whom the investigator (sub investigator) considers ineligible for the study.

Study Plan

This section provides details of the study plan, including how the study is designed and what the study is measuring.

How is the study designed?

Design Details

  • Primary Purpose: Treatment
  • Allocation: N/A
  • Interventional Model: Single Group Assignment
  • Masking: None (Open Label)

Arms and Interventions

Participant Group / Arm
Intervention / Treatment
Experimental: Ropinirole PR/XR
Drug: Ropinirole prolonged release/extended release(PR/XR)
Subjects will take the investigational drug once daily at the same time each day, it is recommended that this is in the morning for optimal benefit. Investigational drug is taken for 52 weeks, starting on the next day of the Week 0 visit. One tablet of ropinirole PR/XR 2 mg tablets will be orally dosed as the initial dose. The dose will be titrated weekly by 2 mg/day, and increased to 8 mg/day in Week 4. From Week 5 up to 16, the dose will be increased at minimum intervals of one week between titration steps until sufficient efficacy is obtained, according to individual clinical response and tolerability (the dose may be titrated up to 16 mg/day). In Week 16 and further, treatment dose at Week 16 will be continuously administered up to Week 52. If insufficient efficacy is judged in a subject during treatment, or unable to maintain the dose due to adverse event, the treatment dose may be changed. The dose is down tapered according to the maintenance dose at Week 52 (or withdrawal).

What is the study measuring?

Primary Outcome Measures

Outcome Measure
Measure Description
Time Frame
Food Effects on Cmax and Cmin of SKF101468 (Ropinirole) and Its Metabolites
Time Frame: Weeks 5-16
The dose of SKF101468 and its metabolites was normalized to 1 mg. Blood sampling at steady state up to 24 hours post dose after receiving the maintenance dose was conducted. In order to investigate the effect of a meal on pharmacokinetics, blood was sampled twice (after a standard morning meal and at fasted state) from identical participants. Cmax: maximum concentration, Cmin: trough plasma concentration.
Weeks 5-16
Food Effects on AUC0-24 of SKF101468 (Ropinirole) and Its Metabolites
Time Frame: Weeks 5-16
The dose of SKF101468 and its metabolites was normalized to 1 mg. Blood sampling at steady state up to 24 hours (hr) post dose after receiving the maintenance dose was conducted. In order to investigate the effect of a meal on pharmacokinetics, blood was sampled twice (after a standard morning meal and at fasted state) from identical participants. AUC0-24: area under the drug concentration 24 hr curve.
Weeks 5-16
Food Effects on Tmax of SKF101468 (Ropinirole) and Its Metabolites
Time Frame: Weeks 5-16
The dose of SKF101468 and its metabolites was normalized to 1 mg. Blood sampling at steady state up to 24 hours post dose after receiving the maintenance dose was conducted. In order to investigate the effect of a meal on pharmacokinetics, blood was sampled twice (after a standard morning meal and at fasted state) from identical participants. Tmax: time of maximum concentration. Data are presented as the median difference between fed and fasted states for ropinirole and each metabolite.
Weeks 5-16
Plasma Trough Concentrations of SKF101468 (Ropinirole) and Its Metabolites
Time Frame: Weeks 1-16
Blood sampling in the fixed titration phase will be performed at 24 hour post dose of the last dose of 2, 4, and 8 mg (immediately before the morning dose). Blood sampling in the maintenance dose phase will be performed at 24 hour post dose of 10 mg or more for one week or longer (immediately before the morning dose), as sampling needs to be conducted at steady state.
Weeks 1-16

Secondary Outcome Measures

Outcome Measure
Measure Description
Time Frame
Total Score in the Japanese UPDRS Part III
Time Frame: Weeks 0-52
The Unified Parkinson's Disease Rating Scale (UPDRS) assesses the status of Parkinson's Disease (PD) patients objectively. The Japanese UPDRS Part III assesses motor examination on 27 items. Participants receive a score of 0-4 points per each item. The maximum total score is 108 points. A higher score indicates more severe PD symptoms.
Weeks 0-52
Change From Baseline in the Japanese UPDRS Part III
Time Frame: Baseline (Week 0) and Weeks 1-52
The UPDRS assesses the status of PD patients objectively. The Japanese UPDRS Part III assesses motor examination on 27 items. Participants receive a score of 0-4 points per each item. The maximum total score is 108 points. A higher score indicates more severe PD symptoms.
Baseline (Week 0) and Weeks 1-52
Percent Change From Baseline in the Japanese UPDRS Part III
Time Frame: Baseline (Week 0) and Weeks 1-52
The UPDRS assesses the status of PD patients objectively. The Japanese UPDRS Part III assesses motor examination on 27 items. Participants receive a score of 0-4 points per each item. A maximum total score is 108 points.The higher score indicates more severe PD symptoms.
Baseline (Week 0) and Weeks 1-52
Percentage of Responders of the Total Score in the Japanese UPDRS Total Score in Part III
Time Frame: Baseline (Week 0) and Weeks 1-52
A responder is defined as a participant with a 30% or more reduction at baseline. The UPDRS assesses the status of PD patients objectively. The Japanese UPDRS Part III assesses motor examination on 27 items. Participants receive a score of 0-4 points per each item. The maximum total score is 108 points. A higher score indicates more severe PD symptoms.
Baseline (Week 0) and Weeks 1-52
Total Score in the Japanese UPDRS Part I
Time Frame: Weeks 0-52
The UPDRS assesses the status of PD patients objectively. The Japanese UPDRS Part I assesses mentation, behavior, and mood on 4 items. Participants receive a score of 0-4 points per each item. The maximum total score is 16 points. A higher score indicates more severe mental symptoms.
Weeks 0-52
Change From Baseline in the Japanese UPDRS Part I
Time Frame: Baseline (Week 0) and Weeks 1-52
The UPDRS (Unified Parkinson's Disease Rating Scale) assesses the status of PD patients objectively. The Japanese UPDRS Part I assesses mentation, behavior, and mood on 4 items. Participants receive a score of 0-4 points per each item. The maximum total score is 16 points. A higher score indicates more severe mental symptoms.
Baseline (Week 0) and Weeks 1-52
Percent Change From Baseline in the Japanese UPDRS Part I
Time Frame: Baseline (Week 0) and Weeks 1-52
The UPDRS (Unified Parkinson's Disease Rating Scale) assesses the status of PD patients objectively. The Japanese UPDRS Part I assesses mentation, behavior, and mood on 4 items. Participants receive a score of 0-4 points per each item. The maximum total score is 16 points. A higher score indicates more severe mental symptoms.
Baseline (Week 0) and Weeks 1-52
Total Score in the Japanese UPDRS Part II
Time Frame: Weeks 0-52
The UPDRS assesses the status of PD patients objectively. The Japanese UPDRS Part II assesses activities of daily living on 13 items. Participants receive a score of 0-4 points per each item. The maximum total score is 52 points. A higher score indicates more severe PD symptoms.
Weeks 0-52
Change From Baseline in the Japanese UPDRS Part II
Time Frame: Baseline (Week 0) and Weeks 1-52
The UPDRS assesses the status of PD patients objectively. The Japanese UPDRS Part II assesses activities of daily living on 13 items. Participants receive a score of 0-4 points per each item. The maximum total score is 52 points. A higher score indicates more severe PD symptoms.
Baseline (Week 0) and Weeks 1-52
Percent Change From Baseline in the Japanese UPDRS Part II
Time Frame: Baseline (Week 0) and Weeks 1-52
The UPDRS assesses the status of PD patients objectively. The Japanese UPDRS Part II assesses activities of daily living on 13 items. Participants receive a score of 0-4 points per each item. The maximum total score is 52 points. A higher score indicates more severe PD symptoms.
Baseline (Week 0) and Weeks 1-52
Total Score in the Japanese UPDRS Part IV
Time Frame: Baseline (Week 0) and Weeks 0-52
The UPDRS assesses the status of PD patients objectively. The Japanese UPDRS Part IV assesses complications of therapy on 11 items. Participants receive a score of 0-4 or 0-1 points per each item depending on the item. The maximum total score is 23 points. A higher score indicates more severe symptoms of complications.
Baseline (Week 0) and Weeks 0-52
Change From Baseline in the Japanese UPDRS Part IV
Time Frame: Baseline (Week 0) and Weeks 1-52
The UPDRS assesses the status of PD patients objectively. The Japanese UPDRS Part IV assesses complications of therapy on 11 items. Participants receive a score of 0-4 or 0-1 points per each item depending on the item. The maximum total score is 23 points. A higher score indicates more severe symptoms of complications.
Baseline (Week 0) and Weeks 1-52
Percent Change From Baseline in the Japanese UPDRS Part IV
Time Frame: Baseline (Week 0) and Weeks 1-52
The UPDRS assesses the status of PD patients objectively. The Japanese UPDRS Part IV assesses complications of therapy on 11 items. Participants receive a score of 0-4 or 0-1 points per each item depending on the item. The maximum total score is 23 points. A higher score indicates more severe symptoms of complications.
Baseline (Week 0) and Weeks 1-52
Summary of the Modified Hoehn & Yahr Criteria Stages
Time Frame: Screening-Week 52
Hoehn & Yahr criteria were measured on an 8-point scale. 0: No signs of disease, 1: Unilateral disease, 1.5: Unilateral plus axial involvement, 2: Bilateral disease, 2.5: Mild bilateral disease, 3: Mild to moderate bilateral disease. No subjects evaluated had a score of 4 (severe disability) or 5 (wheelchair bound or bedridden unless aided).
Screening-Week 52
Number of Participants Scored as Responders on the Clinician's Global Impression (CGI) Scale
Time Frame: Weeks 1-52
CGI is measured on a 7-point scale. 1: Very much improved, 2: Much Improved, 3: Minimally improved, 4: No change, 5: Minimally worse, 6: Much worse, 7: Very much worse. Responders are defined as those participants scored as "very much improved" or "much improved."
Weeks 1-52
Percentage of Participants Who Remained in the Study on the Indicated Days
Time Frame: Days 0-364
The percentage of participants remaining in the study was examined using the Kaplan-Meier method, in which a premature discontinuation will be considered as an event.
Days 0-364
Change From Baseline in Albumin, Total Protein, and Hemoglobin at Weeks 16 and 52
Time Frame: Baseline (Screening) and Weeks 16 and 52
Change from baseline was calculated as the Week 16 and 52 values minus the baseline values.
Baseline (Screening) and Weeks 16 and 52
Change From Baseline in Alkaline Phosphatase, Alanine Amino Transferase, Aspartate Amino Transferase, Creatine Kinase, Gamma Glutamyl Transferase, and Lactate Dehydrogenase at Weeks 16 and 52
Time Frame: Baseline (Screening) and Weeks 16 and 52
Change from baseline was calculated as the Week 16 and 52 values minus the baseline values.
Baseline (Screening) and Weeks 16 and 52
Change From Baseline in Total Bilirubin, Blood Urea Nitrogen, and Creatinine at Weeks 16 and 52
Time Frame: Baseline (Screening) and Weeks 16 and 52
Change from baseline was calculated as the Week 16 and 52 values minus the baseline values.
Baseline (Screening) and Weeks 16 and 52
Change From Baseline in Blood Urea Nitrogen, Cholesterol, Chloride, Potassium, and Sodium at Weeks 16 and 52
Time Frame: Baseline (Screening) and Weeks 16 and 52
Change from baseline was calculated as the Week 16 and 52 values minus the baseline values.
Baseline (Screening) and Weeks 16 and 52
Change From Baseline in Prolactin at Weeks 16 and 52
Time Frame: Baseline (Screening) and Weeks 16 and 52
Change from baseline was calculated as the Week 16 and 52 values minus the baseline values.
Baseline (Screening) and Weeks 16 and 52
Change From Baseline in Hematocrit at Weeks 16 and 52
Time Frame: Baseline (Screening) and Weeks 16 and 52
Change from baseline was calculated as the Week 16 and 52 values minus the baseline values.
Baseline (Screening) and Weeks 16 and 52
Change From Baseline in Platelet Count and White Blood Cell Count at Weeks 16 and 52
Time Frame: Baseline (Screening) and Weeks 16 and 52
Change from baseline was calculated as the Week 16 and 52 values minus the baseline values.
Baseline (Screening) and Weeks 16 and 52
Change From Baseline in Red Blood Cell Count at Weeks 16 and 52
Time Frame: Baseline (Screening) and Weeks 16 and 52
Change from baseline was calculated as the Week 16 and 52 values minus the baseline values.
Baseline (Screening) and Weeks 16 and 52
Urinalysis Data
Time Frame: Screening, Week 16, and Week 52
The number of participants with the indicated dipstick test values were measured. Dipstick test values: Neg Value, Trace, +1, +2, +3, +4. No participants had a score of +5.
Screening, Week 16, and Week 52
Number of Participants With the Indicated Shift From Baseline in 12-Lead Electrocardiogram (ECG) Findings at Weeks 16 and 52
Time Frame: Baseline (Screening) and Weeks 16 and 52
Baseline Finding/Time Period Finding. Abbreviations: N = normal; A = abnormal; CS = clinically significant; NCS = not clinically significant. Options include N/N, N/ANCS, N/ACS, ANCS/N, ANCS/ANCS, ANCS/ACS, ACS/N, ACS/ANCS, and ACS/ACS.
Baseline (Screening) and Weeks 16 and 52
Change From Baseline in Supine and Standing Systolic and Diastolic Blood Pressure at Weeks 16 and 52
Time Frame: Baseline (Screening) and Weeks 16 and 52
Change from baseline was calculated as Week 16 and Week 52 values minus baseline values.
Baseline (Screening) and Weeks 16 and 52
Change From Baseline in Supine and Standing Pulse Rate at Weeks 16 and 52
Time Frame: Baseline (Screening) and Weeks 16 and 52
Change from baseline was calculated as Week 16 and Week 52 values minus baseline values.
Baseline (Screening) and Weeks 16 and 52

Collaborators and Investigators

This is where you will find people and organizations involved with this study.

Sponsor

GlaxoSmithKline

Study record dates

These dates track the progress of study record and summary results submissions to ClinicalTrials.gov. Study records and reported results are reviewed by the National Library of Medicine (NLM) to make sure they meet specific quality control standards before being posted on the public website.

Study Major Dates

Study Start

April 9, 2007

Primary Completion (Actual)

March 1, 2009

Study Completion (Actual)

March 10, 2009

Study Registration Dates

First Submitted

February 9, 2007

First Submitted That Met QC Criteria

February 9, 2007

First Posted (Estimate)

February 13, 2007

Study Record Updates

Last Update Posted (Actual)

September 27, 2018

Last Update Submitted That Met QC Criteria

August 30, 2018

Last Verified

August 1, 2018

More Information

Terms related to this study

Keywords

Additional Relevant MeSH Terms

Other Study ID Numbers

  • ROP106064

This information was retrieved directly from the website clinicaltrials.gov without any changes. If you have any requests to change, remove or update your study details, please contact register@clinicaltrials.gov. As soon as a change is implemented on clinicaltrials.gov, this will be updated automatically on our website as well.

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