Parkinson's Disease Clinical Trial
Official title:
A Double-Blind, 3-Arm, Parallel Group, Placebo- and Ropinirole-Controlled Study for SPM 962 in Advanced Parkinson's Disease Patients With Concomitant Treatment of L-dopa
- To demonstrate the non-inferiority of SPM 962 to ropinirole in terms of efficacy in
order to confirm clinical value of SPM 962.
- To demonstrate the superiority of SPM 962 to placebo in terms of efficacy.
- To investigate the tolerability and safety of SPM 962 up to 36.0 mg/day.
| Status | Completed |
| Enrollment | 420 |
| Est. completion date | May 2011 |
| Est. primary completion date | May 2011 |
| Accepts healthy volunteers | No |
| Gender | Both |
| Age group | 30 Years to 79 Years |
| Eligibility |
Inclusion Criteria: - Subject diagnosed as having Parkinson's disease in accordance with "Diagnostic Criteria established by the Research Committee of MHLW-specified Intractable Neurodegenerative Diseases (1995)". - Subject is 30 and more and less than 80 years of age at the time of informed consent. - Hoehn & Yahr stage 2-4 (on time). - Total UPDRS Part 3 score is over 10 at screening test (on time). - Subject is on a stable dose of L-dopa with no change in daily dose or dosing regimen for at least 28 days prior to the initial treatment of SPM 962. - Subject has any of the following problematic symptoms; 1) Wearing off phenomenon (including frozen gait at off time and dystonia at off time) 2) On and off phenomenon 3) Delayed-on and/or No-on phenomenon 4) Dyskinesia 5) Not well controlled with L-dopa. Exclusion Criteria: - Subject who has previously participated in a clinical trial of SPM962 and taken the investigational product (IP). - Subject has psychiatric symptoms, e.g. confusion, hallucination, delusion, excitation, delirium, abnormal behavior at screening test or baseline. - Subject whose SBP declines by at least 30 mmHg from supine to standing position based on the orthostatic hypotension assessment, or subject who develops orthostatic hypotension at baseline. - Subject has a history of epilepsy, convulsion and other. - Subject who has complications or a history of serious cardiac diseases or arrhythmia (eg, congestive heart failure of class 3 or 4 in the NYHA classification, second or third degree atrioventricular block, complete left bundle branch block, sick sinus syndrome, ventricular fibrillation, myocardial infarction within 12 months prior to the screening test, or a complication of angina pectoris). - Subjects has QTc-interval >450 msec twice at screening. Subject has a the average QTc-interval from two ECGs >450 msec in males and >470 msec in females at baseline. - Subject has congenital long QT syndrome. - Subject whose serum potassium level is < 3.5mEq/L at the screening test. - Subject has a total bilirubin >= 3.0 mg/dL or AST(GOT) or ALT(GPT) greater than 2.5 times of the upper limit of the reference range (or >= 100 IU/L) at screening test, or suffers complications of active phase of chronic hepatitis or liver cirrhosis. - Subject has BUN >= 30 mg/dL or serum creatinine >= 2.0 mg/dl at screening test. - Subject has a history of allergic reaction to topical agents such as transdermal patch. - Subject has a history of known intolerance/hypersensitivity to ropinirole and/or adverse drug reactions that prevent subject from receiving treatment. - Subject is pregnant or nursing or woman who plans pregnancy during the trial. - Subject is receiving therapy with prohibited drug specified in the study protocol. - Subject has a history of pallidotomy, thalamotomy, deep brain stimulation or fetal tissue transplant. - Subject has dementia, including DLB and PDD (MMSE score <= 24 at screening). - Subject who has a complication or history of malignant neoplastic disease, or received treatment for the disease within 12 months prior to the screening test. - Subject is unable to give consent. - Subject who is unable to properly record information in a diary. - Subject is participating in another trial of IPs or received other IPs within 12 weeks prior to commencement of study treatment. - Investigator judges that subject is inappropriate as a study subject with other reasons. |
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment
| Country | Name | City | State |
|---|---|---|---|
| n/a | |||
| Lead Sponsor | Collaborator |
|---|---|
| Otsuka Pharmaceutical Co., Ltd. |
Japan,
| Type | Measure | Description | Time frame | Safety issue |
|---|---|---|---|---|
| Primary | Unified Parkinson's Disease Rating Score (UPDRS) Part 3 Sum Score | Mean change (LOCF) from baseline in UPDRS Part 3 sum score (on state) at 16 weeks after dosing. UPDRS is a scale for monitoring Parkinson's Disease-related disability and impairment. The UPDRS consists of the following four sub-scales. Part 1: Mentation, Part 2: Activities of Daily Living, Part 3: Motor, Part 4: Complications. Part 3 assesses 14 items. Each item is scored from 0 (normal) to 4 (severe). The sum score serves as the sub-scale score. A higher score indicates a greater severity of symptoms. Thus a decrease in the scores means improvement. |
baseline, 16 weeks after dosing | No |
| Secondary | UPDRS Part 3 Sum Score | Mean change (LOCF) from baseline in UPDRS Part 3 sum score (on state) at 8 and 10 weeks after dosing. UPDRS Part 3 assesses 14 items. Each item is scored from 0 (normal) to 4 (severe). The sum score serves as the sub-scale score. A higher score indicates a greater severity of symptoms. Thus a decrease in the scores means improvement. |
baseline, 8 and 10 weeks after dosing | No |
| Secondary | UPDRS Part 2 Sum Score | Mean change (LOCF) from baseline in UPDRS Part 2 sum score (average scores of on state and off state) at 16 weeks after dosing. UPDRS 2 assesses 13 items. Each item is scored from 0 (normal) to 4 (severe). The sum score serves as the sub-scale score. A higher score indicates a greater severity of symptoms. Thus a decrease in the scores means improvement. |
Baseline, 16 weeks after dosing | No |
| Secondary | Off Time | Mean change (LOCF) from baseline in off time at 16 weeks after dosing. Off-time is a state where L-Dopa becomes ineffective. Off-time was measured by patient diary in hours/day. | Baseline, 16 weeks after dosing | No |
| Secondary | Parkinson's Disease Sleep Scale-2 (PDSS-2) | Mean change (LOCF) from baseline in PDSS-2 sum score at 16 weeks after dosing. PDSS-2 is a scale for assessing sleep disorders in Parkinson's disease. PDSS consists of 15 questions about sleep and nocturnal disturbances. The score of each question ranges from 0 (never) to 4 (very frequent). The sum of each question serves as the scale score. Thus a decrease in the scores means improvement. | Baseline, 16 weeks after dosing | No |
| Secondary | On Time | Mean change (LOCF) from baseline in on time at 16 weeks after dosing. On-time is a state where L-Dopa is effective. On-time was measured by patient diary in hours/day. | Baseline, 16 weeks after dosing | No |
| Secondary | On Time Without Dyskinesia Disturbing Daily Activities | Mean change (LOCF) from baseline in on time without dyskinesia disturbing daily activities at 16 weeks after dosing. On-time is a state where L-Dopa is effective. On-time was measured by patient diary in hours/day. |
Baseline, 16 weeks after dosing | No |
| Secondary | On Time With Dyskinesia Disturbing Daily Activities | Mean change (LOCF) from baseline in on time with dyskinesia disturbing daily activities at 16 weeks after dosing (rate against on time). | Baseline, 16 weeks after dosing | No |
| Secondary | Effective Rate in UPDRS Part 3 Sum Score | Effective rate (percentage of subjects with 20% or 30% decrease) (LOCF) in UPDRS Part 3 sum score (on state) at 16 weeks after dosing. | Baseline, 16 weeks after dosing | No |
| Secondary | Effective Rate in UPDRS Part 2 Sum Score | Effective rate (percentage of subjects with 20% or 30% decrease) (LOCF) in UPDRS Part 2 sum score (average scores of on state and off state) at 16 weeks after dosing. | Baseline, 16 weeks after dosing | No |
| Secondary | Effective Rate in Off Time | Effective rate (percentage of subjects with 20% or 30% decrease) (LOCF) in off time at 16 weeks after dosing. On-time is a state where L-Dopa is effective. On-time was measured by patient diary in hours/day. |
Baseline, 16 weeks after dosing | No |
| Secondary | Clinical Global Impression (CGI) | Change (LOCF) from baseline in CGI score. CGI improvement is a clinician-reported scale for assessing how much the patient's illness has improved or worsened from baseline. The scale scoring criteria are 1: very much improved, 2: much improved, 3: minimally improved, 4: no change, 5: minimally worse, 6: much worse, 7: very much worse. A decrease in the scores means improvement. |
Baseline, 16 weeks after dosing | No |
| Secondary | Dystonia (at an Early Hour) | Change (LOCF) from baseline in occurrence of Dystonia (at an early hour). | Baseline, 16 weeks after dosing | No |
| Secondary | Dystonia (in the Daytime) | Change (LOCF) from baseline in occurrence of Dystonia (in the daytime). | Baseline, 16 weeks after dosing | No |
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