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Safinamide in Levodopa Induced Dyskinesia in Parkinson's Disease Subjects (Safinamide-LID)

Primary Purpose

Parkinson's Disease

Status
Completed
Phase
Phase 2
Locations
International
Study Type
Interventional
Intervention
Placebo
Safinamide
Sponsored by
Newron Pharmaceuticals SPA
About
Eligibility
Locations
Arms
Outcomes
Full info

About this trial

This is an interventional supportive care trial for Parkinson's Disease focused on measuring Safinamide - Parkinson's disease - Levodopa induced dyskinesia, Advanced idiopathic PD patients treated with L-dopa and suffering from temporally predictable L-dopa induced peak-dose dyskinesia.

Eligibility Criteria

30 Years - undefined (Adult, Older Adult)All SexesDoes not accept healthy volunteers

Inclusion Criteria:

  1. The subject has given his/her written informed consent to participate in the trial.
  2. The subject presents with a diagnosis of idiopathic Parkinson's disease according to the United Kingdom (UK) Parkinson's Disease Society Brain Bank Clinical Diagnosis Criteria
  3. The subject is an out-patient aged 30 years or above.
  4. PD subjects with a Hoehn and Yahr disease staging of II-IV (in the ON state).
  5. PD subjects experiencing levodopa induced dyskinesias, specifically predictable peak-dose dyskinesia.
  6. Peak-dose dyskinesia must be considered by the subject to be problematic and/or disabling.
  7. Peak-dose dyskinesia must warrant medical treatment in the Investigator's opinion.
  8. The subject has participated successfully in a diary-card training session.
  9. In the judgment of the Investigator based on the subject's history, previous treatments, and the clinical presentation, the subject is considered as being optimally treated at screening (i.e., further adjustments of current medication will not further improve the subject's symptoms of Parkinson's disease).
  10. Stable dose of PD drugs for at least 4 weeks before Screening Visit. This may include: levodopa dopamine agonists, c-ortho methyl transferase (COMT) inhibitors, and anticholinergics.
  11. The dose of levodopa and all PD drugs used during the trial must remain unchanged throughout the trial.
  12. Female subjects must be neither pregnant or breast-feeding and must lack child-bearing potential, as defined either by:

    1. be either post menopausal for at least 2 years , surgically sterilised or have undergone hysterectomy, or
    2. if of child bearing potential, be willing to avoid pregnancy by using an adequate method of contraception for four weeks prior to, during and four weeks after the last dose of trial medication. For the purposes of this trial, women of childbearing potential are defined as all female subjects after puberty unless they are post-menopausal for at least two years, are surgically sterile or are sexually inactive.
  13. The subject shows adequate compliance with the schedule for intake of trial medication and the completion of the diaries.

Exclusion Criteria:

  1. The subject has participated in any safinamide clinical trial before.
  2. The subject is experiencing exclusively diphasic, off state, myoclonic, dystonic, or akathetic dyskinesias without peak dose dyskinesia.
  3. (For female subjects) The subject is pregnant or lactating.
  4. Treatment with a MAO-B inhibitor within the eight weeks prior to the screening visit.
  5. Treatment with amantadine in the four weeks prior to the screening visit or budipine in the eight weeks prior to the screening visit.
  6. Treatment with opioids (e.g., tramadol, meperidine derivatives), serotonin norepinephrine reuptake inhibitors (SNRIs) (e.g. venlafaxine, duloxetine), tri- or tetra-cyclic antidepressants, in the past 8 weeks prior to the screening visit. Dextromethorphan will be permitted if used for treating cough.
  7. The subject has received neurosurgical intervention related to PD (e.g. deep brain stimulation, thalamotomy etc.) or is scheduled to do so during the trial period.
  8. Current clinically significant gastro-intestinal, renal, hepatic, endocrine, pulmonary or cardiovascular disease, including acute gastric ulcer, hypertension that is not well controlled, asthma, chronic obstructive pulmonary disease (COPD), and unstable Type I diabetes. Subjects with a history of gastric ulcer who have not had a recent episode of acute gastritis and are not currently experiencing gastric pain will be eligible for inclusion.
  9. Neoplastic disorder, which is either currently active or has been in remission for less than one year.
  10. Diagnosis of HIV, or positive test for Hepatitis C antibodies, or Hepatitis B surface antigen.
  11. Concomitant disease likely to interfere with trial medication (e.g. capable of altering absorption, metabolism, or elimination of the trial drug).
  12. The subject has any clinically significant illness that, in the Investigator's opinion, might interfere with the subject's ability to participate in the trial.
  13. Second- or third-degree atrio-ventricular block or sick sinus syndrome, uncontrolled atrial fibrillation, severe or unstable angina, congestive heart failure, myocardial infarction within 3 months of the screening visit, or a significant ECG abnormality, including corrected QT interval (QTc) - 450 msec (males) or - 470 msec (females), where QTc is based on Bazett's correction method.
  14. Ophthalmologic history including any of the following conditions: albino subjects, family history of hereditary retinal disease, progressive and/or severe diminution of visual acuity (i.e., 20/70), retinitis pigmentosa, retinal pigmentation due to any cause, any active retinopathy or ocular inflammation (uveitis), or diabetic retinopathy
  15. The subject is suffering from any dementia or other psychiatric illness that prevents him/her from giving informed consent, i.e. Montreal Cognitive Assessment (MoCA) <23 points.
  16. Signs and symptoms suggestive of transmissible spongiform encephalopathy, or family members who suffer(ed) from such.
  17. Known hypersensitivity to the trial treatment(s), including placebo or other comparator drug(s).
  18. The subject has legal incapacity or limited legal capacity.
  19. The subject is participating in another clinical trial or has done so within the past 30 days
  20. Treatment with a drug that has hepatotoxic potential, e.g., tamoxifen, within 4 weeks, or received radiation therapy or a drug with cytotoxic potential, e.g, chemotherapy, within one year prior to the screening visit.
  21. Subjects with current diagnosis of substance abuse (DSM-IV) or history of alcohol or drug abuse in the past three months.

Sites / Locations

  • Medical University Graz, Klinische Abteilung für Spezielle Neurologie
  • Medical University Innsbruck, Dept. of Neurology
  • Quebec Memory and Motor Skills Disorders
  • Hôpital Roger Sallengro
  • CIC-Hospital Purpan
  • Neurologie Berlin Praxen
  • St. Josef Hospital, Klinik für Neurologie
  • Facharzt für Neurologie und Psychiatrie
  • Medical and Dental center (ZAF)
  • Sunninghill Hospital
  • Willows Medical Centre

Arms of the Study

Arm 1

Arm 2

Arm Type

Placebo Comparator

Active Comparator

Arm Label

Placebo

Safinamide

Arm Description

Outcomes

Primary Outcome Measures

The maximum reduction in Unified Dyskinesia Rating Score (UDysRS) compared to baseline across all post-baseline dose visits.

Secondary Outcome Measures

Complete new Movement Disorder Society - Unified Parkinson Disease Rating Scale (MDS-UPDRS) and subscales
Complete new Movement Disorder Society - Unified Parkinson Disease Rating Scale (MDS-UPDRS) and subscales
Complete new Movement Disorder Society - Unified Parkinson Disease Rating Scale (MDS-UPDRS) and subscales
Complete new Movement Disorder Society - Unified Parkinson Disease Rating Scale (MDS-UPDRS) and subscales
Complete new Movement Disorder Society - Unified Parkinson Disease Rating Scale (MDS-UPDRS) and subscales
Complete new Movement Disorder Society - Unified Parkinson Disease Rating Scale (MDS-UPDRS) and subscales
Unified Dyskinesia Rating Scale (UDysRS) and subscales (historical and objective)
Unified Dyskinesia Rating Scale (UDysRS) and subscales (historical and objective)
Unified Dyskinesia Rating Scale (UDysRS) and subscales (historical and objective)
Unified Dyskinesia Rating Scale (UDysRS) and subscales (historical and objective)
Unified Dyskinesia Rating Scale (UDysRS) and subscales (historical and objective)
Unified Dyskinesia Rating Scale (UDysRS) and subscales (historical and objective)
Patient's diary (Hauser diary, all parts)
Hauser patient diary: daily total "on" time (ON w/o dyskinesia, or ON with non-troublesome dyskinesia), and daily total "off" time as measured by the patients' diary over the study period.
Patient's diary (Hauser diary, all parts)
Hauser patient diary: daily total "on" time (ON w/o dyskinesia, or ON with non-troublesome dyskinesia), and daily total "off" time as measured by the patients' diary over the study period.
Patient's diary (Hauser diary, all parts)
Hauser patient diary: daily total "on" time (ON w/o dyskinesia, or ON with non-troublesome dyskinesia), and daily total "off" time as measured by the patients' diary over the study period.
Patient's diary (Hauser diary, all parts)
Hauser patient diary: daily total "on" time (ON w/o dyskinesia, or ON with non-troublesome dyskinesia), and daily total "off" time as measured by the patients' diary over the study period.
Patient's diary (Hauser diary, all parts)
Hauser patient diary: daily total "on" time (ON w/o dyskinesia, or ON with non-troublesome dyskinesia), and daily total "off" time as measured by the patients' diary over the study period.
Patient's diary (Hauser diary, all parts)
Hauser patient diary: daily total "on" time (ON w/o dyskinesia, or ON with non-troublesome dyskinesia), and daily total "off" time as measured by the patients' diary over the study period.
Parkinson's Disease Dyskinesia Scale (PDYS-26) (dyskinesia specific Activities of Daily Living (ADL) questionnaire)
Parkinson's Disease Dyskinesia Scale (PDYS-26) (dyskinesia specific Activities of Daily Living (ADL) questionnaire)
Parkinson's Disease Dyskinesia Scale (PDYS-26) (dyskinesia specific Activities of Daily Living (ADL) questionnaire)
Parkinson's Disease Dyskinesia Scale (PDYS-26) (dyskinesia specific Activities of Daily Living (ADL) questionnaire)
Parkinson's Disease Dyskinesia Scale (PDYS-26) (dyskinesia specific Activities of Daily Living (ADL) questionnaire)
Parkinson's Disease Dyskinesia Scale (PDYS-26) (dyskinesia specific Activities of Daily Living (ADL) questionnaire)
Clinical Global Impression (CGI) (dyskinesia specific)
Scales measure the overall impression both the investigator and the patient have about the subject's general health. This is measured at baseline and the impression of change versus is measured at each visit. Here we are measuring efficacy.
Clinical Global Impression (CGI) (dyskinesia specific)
Scales measure the overall impression both the investigator and the patient have about the subject's general health. This is measured at baseline and the impression of change versus is measured at each visit. Here we are measuring efficacy.
Clinical Global Impression (CGI) (dyskinesia specific)
Scales measure the overall impression both the investigator and the patient have about the subject's general health. This is measured at baseline and the impression of change versus is measured at each visit. Here we are measuring efficacy.
Clinical Global Impression (CGI) (dyskinesia specific)
Scales measure the overall impression both the investigator and the patient have about the subject's general health. This is measured at baseline and the impression of change versus is measured at each visit. Here we are measuring efficacy.
Clinical Global Impression (CGI) (dyskinesia specific)
Scales measure the overall impression both the investigator and the patient have about the subject's general health. This is measured at baseline and the impression of change versus is measured at each visit. Here we are measuring efficacy.
Clinical Global Impression (CGI) (dyskinesia specific)
Scales measure the overall impression both the investigator and the patient have about the subject's general health. This is measured at baseline and the impression of change versus is measured at each visit. Here we are measuring efficacy.
Patient Global Impression (PGI) (dyskinesia specific)
Scales measure the overall impression both the investigator and the patient have about the subject's general health. This is measured at baseline and the impression of change versus is measured at each visit. Here we are measuring efficacy.
Patient Global Impression (PGI) (dyskinesia specific)
Scales measure the overall impression both the investigator and the patient have about the subject's general health. This is measured at baseline and the impression of change versus is measured at each visit. Here we are measuring efficacy.
Patient Global Impression (PGI) (dyskinesia specific)
Scales measure the overall impression both the investigator and the patient have about the subject's general health. This is measured at baseline and the impression of change versus is measured at each visit. Here we are measuring efficacy.
Patient Global Impression (PGI) (dyskinesia specific)
Scales measure the overall impression both the investigator and the patient have about the subject's general health. This is measured at baseline and the impression of change versus is measured at each visit. Here we are measuring efficacy.
Patient Global Impression (PGI) (dyskinesia specific)
Scales measure the overall impression both the investigator and the patient have about the subject's general health. This is measured at baseline and the impression of change versus is measured at each visit. Here we are measuring efficacy.
Patient Global Impression (PGI) (dyskinesia specific)
Scales measure the overall impression both the investigator and the patient have about the subject's general health. This is measured at baseline and the impression of change versus is measured at each visit. Here we are measuring efficacy.

Full Information

First Posted
April 8, 2010
Last Updated
March 28, 2013
Sponsor
Newron Pharmaceuticals SPA
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1. Study Identification

Unique Protocol Identification Number
NCT01113320
Brief Title
Safinamide in Levodopa Induced Dyskinesia in Parkinson's Disease Subjects
Acronym
Safinamide-LID
Official Title
A Double-blind, Randomized, Placebo-controlled, Parallel-group, Dose Escalation Trial to Explore the Potential Antidyskinetic Properties of Safinamide in Patients With Parkinson's Disease Suffering From Levodopa Induced Dyskinesias
Study Type
Interventional

2. Study Status

Record Verification Date
January 2012
Overall Recruitment Status
Completed
Study Start Date
April 2010 (undefined)
Primary Completion Date
November 2011 (Actual)
Study Completion Date
January 2012 (Actual)

3. Sponsor/Collaborators

Responsible Party, by Official Title
Sponsor
Name of the Sponsor
Newron Pharmaceuticals SPA

4. Oversight

Data Monitoring Committee
No

5. Study Description

Brief Summary
Approximately twenty four (24) subjects will participate in this research trial. The research trial will be conducted in approximately twelve (12) medical centers in the following countries: Germany, France, South Africa, Austria and Canada. The research trial will last until December 2011.

6. Conditions and Keywords

Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study
Parkinson's Disease
Keywords
Safinamide - Parkinson's disease - Levodopa induced dyskinesia, Advanced idiopathic PD patients treated with L-dopa and suffering from temporally predictable L-dopa induced peak-dose dyskinesia.

7. Study Design

Primary Purpose
Supportive Care
Study Phase
Phase 2
Interventional Study Model
Parallel Assignment
Masking
ParticipantCare ProviderInvestigatorOutcomes Assessor
Allocation
Randomized
Enrollment
26 (Actual)

8. Arms, Groups, and Interventions

Arm Title
Placebo
Arm Type
Placebo Comparator
Arm Title
Safinamide
Arm Type
Active Comparator
Intervention Type
Drug
Intervention Name(s)
Placebo
Intervention Description
Evaluable dose levels are 100 mg (8 days), 200 mg (10 days), and 300 mg (42 days). Intermediate dose levels are 150 mg (Study days 9-11) and 250 mg (Study days 23-25) and have a duration of three days. Safinamide and identical Placebo will be provided in tablets equivalent of 50 mg in blisters. Dosing will be achieved using appropriate multiples of these tablet strengths
Intervention Type
Drug
Intervention Name(s)
Safinamide
Intervention Description
Evaluable dose levels are 100 mg (8 days), 200 mg (10 days), and 300 mg (42 days). Intermediate dose levels are 150 mg (Study days 9-11) and 250 mg (Study days 23-25) and have a duration of three days. Safinamide will be provided in tablets of 50 mg in blisters. Dosing will be achieved using appropriate multiples of these tablet strengths
Primary Outcome Measure Information:
Title
The maximum reduction in Unified Dyskinesia Rating Score (UDysRS) compared to baseline across all post-baseline dose visits.
Time Frame
Day 66
Secondary Outcome Measure Information:
Title
Complete new Movement Disorder Society - Unified Parkinson Disease Rating Scale (MDS-UPDRS) and subscales
Time Frame
At each individual post-dose visit: Baseline
Title
Complete new Movement Disorder Society - Unified Parkinson Disease Rating Scale (MDS-UPDRS) and subscales
Time Frame
At each individual post-dose visit: Day 8
Title
Complete new Movement Disorder Society - Unified Parkinson Disease Rating Scale (MDS-UPDRS) and subscales
Time Frame
At each individual post-dose visit: Day 22
Title
Complete new Movement Disorder Society - Unified Parkinson Disease Rating Scale (MDS-UPDRS) and subscales
Time Frame
At each individual post-dose visit: Day 36
Title
Complete new Movement Disorder Society - Unified Parkinson Disease Rating Scale (MDS-UPDRS) and subscales
Time Frame
At each individual post-dose visit: Day 66
Title
Complete new Movement Disorder Society - Unified Parkinson Disease Rating Scale (MDS-UPDRS) and subscales
Time Frame
At each individual post-dose visit: Day 101
Title
Unified Dyskinesia Rating Scale (UDysRS) and subscales (historical and objective)
Time Frame
At each individual visit: Baseline
Title
Unified Dyskinesia Rating Scale (UDysRS) and subscales (historical and objective)
Time Frame
At each individual visit: Day 8
Title
Unified Dyskinesia Rating Scale (UDysRS) and subscales (historical and objective)
Time Frame
At each individual visit: Day 22
Title
Unified Dyskinesia Rating Scale (UDysRS) and subscales (historical and objective)
Time Frame
At each individual visit: Day 36
Title
Unified Dyskinesia Rating Scale (UDysRS) and subscales (historical and objective)
Time Frame
At each individual visit: Day 66
Title
Unified Dyskinesia Rating Scale (UDysRS) and subscales (historical and objective)
Time Frame
At each individual visit: Day 101
Title
Patient's diary (Hauser diary, all parts)
Description
Hauser patient diary: daily total "on" time (ON w/o dyskinesia, or ON with non-troublesome dyskinesia), and daily total "off" time as measured by the patients' diary over the study period.
Time Frame
At each trial visit: Baseline
Title
Patient's diary (Hauser diary, all parts)
Description
Hauser patient diary: daily total "on" time (ON w/o dyskinesia, or ON with non-troublesome dyskinesia), and daily total "off" time as measured by the patients' diary over the study period.
Time Frame
At each trial visit: Day 8
Title
Patient's diary (Hauser diary, all parts)
Description
Hauser patient diary: daily total "on" time (ON w/o dyskinesia, or ON with non-troublesome dyskinesia), and daily total "off" time as measured by the patients' diary over the study period.
Time Frame
At each trial visit: Day 22
Title
Patient's diary (Hauser diary, all parts)
Description
Hauser patient diary: daily total "on" time (ON w/o dyskinesia, or ON with non-troublesome dyskinesia), and daily total "off" time as measured by the patients' diary over the study period.
Time Frame
At each trial visit: Day 36
Title
Patient's diary (Hauser diary, all parts)
Description
Hauser patient diary: daily total "on" time (ON w/o dyskinesia, or ON with non-troublesome dyskinesia), and daily total "off" time as measured by the patients' diary over the study period.
Time Frame
At each trial visit: Day 66
Title
Patient's diary (Hauser diary, all parts)
Description
Hauser patient diary: daily total "on" time (ON w/o dyskinesia, or ON with non-troublesome dyskinesia), and daily total "off" time as measured by the patients' diary over the study period.
Time Frame
At each trial visit: Day 101
Title
Parkinson's Disease Dyskinesia Scale (PDYS-26) (dyskinesia specific Activities of Daily Living (ADL) questionnaire)
Time Frame
At each trial visit: Baseline
Title
Parkinson's Disease Dyskinesia Scale (PDYS-26) (dyskinesia specific Activities of Daily Living (ADL) questionnaire)
Time Frame
At each trial visit: Day 8
Title
Parkinson's Disease Dyskinesia Scale (PDYS-26) (dyskinesia specific Activities of Daily Living (ADL) questionnaire)
Time Frame
At each trial visit: Day 22
Title
Parkinson's Disease Dyskinesia Scale (PDYS-26) (dyskinesia specific Activities of Daily Living (ADL) questionnaire)
Time Frame
At each trial visit: Day 36
Title
Parkinson's Disease Dyskinesia Scale (PDYS-26) (dyskinesia specific Activities of Daily Living (ADL) questionnaire)
Time Frame
At each trial visit: Day 66
Title
Parkinson's Disease Dyskinesia Scale (PDYS-26) (dyskinesia specific Activities of Daily Living (ADL) questionnaire)
Time Frame
At each trial visit: Day 101
Title
Clinical Global Impression (CGI) (dyskinesia specific)
Description
Scales measure the overall impression both the investigator and the patient have about the subject's general health. This is measured at baseline and the impression of change versus is measured at each visit. Here we are measuring efficacy.
Time Frame
At each trial visit: Baseline
Title
Clinical Global Impression (CGI) (dyskinesia specific)
Description
Scales measure the overall impression both the investigator and the patient have about the subject's general health. This is measured at baseline and the impression of change versus is measured at each visit. Here we are measuring efficacy.
Time Frame
At each trial visit: Day 8
Title
Clinical Global Impression (CGI) (dyskinesia specific)
Description
Scales measure the overall impression both the investigator and the patient have about the subject's general health. This is measured at baseline and the impression of change versus is measured at each visit. Here we are measuring efficacy.
Time Frame
At each trial visit: Day 22
Title
Clinical Global Impression (CGI) (dyskinesia specific)
Description
Scales measure the overall impression both the investigator and the patient have about the subject's general health. This is measured at baseline and the impression of change versus is measured at each visit. Here we are measuring efficacy.
Time Frame
At each trial visit: Day 36
Title
Clinical Global Impression (CGI) (dyskinesia specific)
Description
Scales measure the overall impression both the investigator and the patient have about the subject's general health. This is measured at baseline and the impression of change versus is measured at each visit. Here we are measuring efficacy.
Time Frame
At each trial visit: Day 66
Title
Clinical Global Impression (CGI) (dyskinesia specific)
Description
Scales measure the overall impression both the investigator and the patient have about the subject's general health. This is measured at baseline and the impression of change versus is measured at each visit. Here we are measuring efficacy.
Time Frame
At each trial visit: Day 101
Title
Patient Global Impression (PGI) (dyskinesia specific)
Description
Scales measure the overall impression both the investigator and the patient have about the subject's general health. This is measured at baseline and the impression of change versus is measured at each visit. Here we are measuring efficacy.
Time Frame
At each trial visit: Baseline
Title
Patient Global Impression (PGI) (dyskinesia specific)
Description
Scales measure the overall impression both the investigator and the patient have about the subject's general health. This is measured at baseline and the impression of change versus is measured at each visit. Here we are measuring efficacy.
Time Frame
At each trial visit: Day 8
Title
Patient Global Impression (PGI) (dyskinesia specific)
Description
Scales measure the overall impression both the investigator and the patient have about the subject's general health. This is measured at baseline and the impression of change versus is measured at each visit. Here we are measuring efficacy.
Time Frame
At each trial visit: Day 22
Title
Patient Global Impression (PGI) (dyskinesia specific)
Description
Scales measure the overall impression both the investigator and the patient have about the subject's general health. This is measured at baseline and the impression of change versus is measured at each visit. Here we are measuring efficacy.
Time Frame
At each trial visit: Day 36
Title
Patient Global Impression (PGI) (dyskinesia specific)
Description
Scales measure the overall impression both the investigator and the patient have about the subject's general health. This is measured at baseline and the impression of change versus is measured at each visit. Here we are measuring efficacy.
Time Frame
At each trial visit: Day 66
Title
Patient Global Impression (PGI) (dyskinesia specific)
Description
Scales measure the overall impression both the investigator and the patient have about the subject's general health. This is measured at baseline and the impression of change versus is measured at each visit. Here we are measuring efficacy.
Time Frame
At each trial visit: Day 101

10. Eligibility

Sex
All
Minimum Age & Unit of Time
30 Years
Accepts Healthy Volunteers
No
Eligibility Criteria
Inclusion Criteria: The subject has given his/her written informed consent to participate in the trial. The subject presents with a diagnosis of idiopathic Parkinson's disease according to the United Kingdom (UK) Parkinson's Disease Society Brain Bank Clinical Diagnosis Criteria The subject is an out-patient aged 30 years or above. PD subjects with a Hoehn and Yahr disease staging of II-IV (in the ON state). PD subjects experiencing levodopa induced dyskinesias, specifically predictable peak-dose dyskinesia. Peak-dose dyskinesia must be considered by the subject to be problematic and/or disabling. Peak-dose dyskinesia must warrant medical treatment in the Investigator's opinion. The subject has participated successfully in a diary-card training session. In the judgment of the Investigator based on the subject's history, previous treatments, and the clinical presentation, the subject is considered as being optimally treated at screening (i.e., further adjustments of current medication will not further improve the subject's symptoms of Parkinson's disease). Stable dose of PD drugs for at least 4 weeks before Screening Visit. This may include: levodopa dopamine agonists, c-ortho methyl transferase (COMT) inhibitors, and anticholinergics. The dose of levodopa and all PD drugs used during the trial must remain unchanged throughout the trial. Female subjects must be neither pregnant or breast-feeding and must lack child-bearing potential, as defined either by: be either post menopausal for at least 2 years , surgically sterilised or have undergone hysterectomy, or if of child bearing potential, be willing to avoid pregnancy by using an adequate method of contraception for four weeks prior to, during and four weeks after the last dose of trial medication. For the purposes of this trial, women of childbearing potential are defined as all female subjects after puberty unless they are post-menopausal for at least two years, are surgically sterile or are sexually inactive. The subject shows adequate compliance with the schedule for intake of trial medication and the completion of the diaries. Exclusion Criteria: The subject has participated in any safinamide clinical trial before. The subject is experiencing exclusively diphasic, off state, myoclonic, dystonic, or akathetic dyskinesias without peak dose dyskinesia. (For female subjects) The subject is pregnant or lactating. Treatment with a MAO-B inhibitor within the eight weeks prior to the screening visit. Treatment with amantadine in the four weeks prior to the screening visit or budipine in the eight weeks prior to the screening visit. Treatment with opioids (e.g., tramadol, meperidine derivatives), serotonin norepinephrine reuptake inhibitors (SNRIs) (e.g. venlafaxine, duloxetine), tri- or tetra-cyclic antidepressants, in the past 8 weeks prior to the screening visit. Dextromethorphan will be permitted if used for treating cough. The subject has received neurosurgical intervention related to PD (e.g. deep brain stimulation, thalamotomy etc.) or is scheduled to do so during the trial period. Current clinically significant gastro-intestinal, renal, hepatic, endocrine, pulmonary or cardiovascular disease, including acute gastric ulcer, hypertension that is not well controlled, asthma, chronic obstructive pulmonary disease (COPD), and unstable Type I diabetes. Subjects with a history of gastric ulcer who have not had a recent episode of acute gastritis and are not currently experiencing gastric pain will be eligible for inclusion. Neoplastic disorder, which is either currently active or has been in remission for less than one year. Diagnosis of HIV, or positive test for Hepatitis C antibodies, or Hepatitis B surface antigen. Concomitant disease likely to interfere with trial medication (e.g. capable of altering absorption, metabolism, or elimination of the trial drug). The subject has any clinically significant illness that, in the Investigator's opinion, might interfere with the subject's ability to participate in the trial. Second- or third-degree atrio-ventricular block or sick sinus syndrome, uncontrolled atrial fibrillation, severe or unstable angina, congestive heart failure, myocardial infarction within 3 months of the screening visit, or a significant ECG abnormality, including corrected QT interval (QTc) - 450 msec (males) or - 470 msec (females), where QTc is based on Bazett's correction method. Ophthalmologic history including any of the following conditions: albino subjects, family history of hereditary retinal disease, progressive and/or severe diminution of visual acuity (i.e., 20/70), retinitis pigmentosa, retinal pigmentation due to any cause, any active retinopathy or ocular inflammation (uveitis), or diabetic retinopathy The subject is suffering from any dementia or other psychiatric illness that prevents him/her from giving informed consent, i.e. Montreal Cognitive Assessment (MoCA) <23 points. Signs and symptoms suggestive of transmissible spongiform encephalopathy, or family members who suffer(ed) from such. Known hypersensitivity to the trial treatment(s), including placebo or other comparator drug(s). The subject has legal incapacity or limited legal capacity. The subject is participating in another clinical trial or has done so within the past 30 days Treatment with a drug that has hepatotoxic potential, e.g., tamoxifen, within 4 weeks, or received radiation therapy or a drug with cytotoxic potential, e.g, chemotherapy, within one year prior to the screening visit. Subjects with current diagnosis of substance abuse (DSM-IV) or history of alcohol or drug abuse in the past three months.
Overall Study Officials:
First Name & Middle Initial & Last Name & Degree
Jonathan Willmer, MD
Organizational Affiliation
Merck Serono S.A., Geneva
Official's Role
Study Director
Facility Information:
Facility Name
Medical University Graz, Klinische Abteilung für Spezielle Neurologie
City
Graz
Country
Austria
Facility Name
Medical University Innsbruck, Dept. of Neurology
City
Innsbruck
Country
Austria
Facility Name
Quebec Memory and Motor Skills Disorders
City
Quebec
Country
Canada
Facility Name
Hôpital Roger Sallengro
City
Lille
Country
France
Facility Name
CIC-Hospital Purpan
City
Toulouse
Country
France
Facility Name
Neurologie Berlin Praxen
City
Berlin
Country
Germany
Facility Name
St. Josef Hospital, Klinik für Neurologie
City
Bochum
Country
Germany
Facility Name
Facharzt für Neurologie und Psychiatrie
City
Düsseldorf
Country
Germany
Facility Name
Medical and Dental center (ZAF)
City
Johannesbourg
Country
South Africa
Facility Name
Sunninghill Hospital
City
Johannesburg
Country
South Africa
Facility Name
Willows Medical Centre
City
Pretoria
Country
South Africa

12. IPD Sharing Statement

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Safinamide in Levodopa Induced Dyskinesia in Parkinson's Disease Subjects

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