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A Phase 2 Clinical Study in Subjects With Primary Progressive Multiple Sclerosis to Assess the Efficacy, Safety and Tolerability of Two Oral Doses of Laquinimod Either of 0.6 mg/Day or 1.5mg/Day (Experimental Drug) as Compared to Placebo (ARPEGGIO)

Primary Purpose

Primary Progressive Multiple Sclerosis

Status
Completed
Phase
Phase 2
Locations
International
Study Type
Interventional
Intervention
Placebo
Laquinimod
Placebo
Sponsored by
Teva Branded Pharmaceutical Products R&D, Inc.
About
Eligibility
Locations
Arms
Outcomes
Full info

About this trial

This is an interventional treatment trial for Primary Progressive Multiple Sclerosis focused on measuring multiple sclerosis, primary progressive multiple sclerosis, oral immunomodulator

Eligibility Criteria

25 Years - 55 Years (Adult)All SexesDoes not accept healthy volunteers

Inclusion Criteria:

  1. Patients must have a confirmed and documented PPMS diagnosis as defined by the 2010 Revised McDonald criteria
  2. Baseline magnetic resonance imaging (MRI) showing lesions consistent with PPMS in either or both brain and spinal cord
  3. Patients must have an Expanded Disability Status Scale (EDSS) score of 3 to 6.5, inclusive, at both screening and baseline visits
  4. Documented evidence of clinical disability progression in the 2 years prior to screening.
  5. Functional System Score (FSS) of > or equal 2 for the pyramidal system or gait impairment due to lower extremity dysfunction
  6. Patients must be between 25 to 55 years of age, inclusive
  7. Women of child-bearing potential must practice an acceptable method of birth control for 30 days before taking the study drug, and 2 acceptable methods of birth control during all study duration and until 30 days after the last dose of treatment is administered.
  8. Patients must sign and date a written informed consent prior to entering the study.
  9. Patients must be willing and able to comply with the protocol requirements for the duration of the study.

Exclusion Criteria:

  1. Patients with history of any multiple sclerosis (MS) exacerbations or relapses, including any episodes of optic neuritis.
  2. Progressive neurological disorder other than PPMS.
  3. Any MRI record showing presence of cervical cord compression.
  4. Baseline MRI showing other findings (including lesions that are atypical for PPMS) that may explain the clinical signs and symptoms.
  5. Relevant history of vitamin B12 deficiency.
  6. Positive human T-lymphotropic virus Type I and II (HTLV-I/II) serology.
  7. Use of experimental or investigational drugs in a clinical study within 24 weeks prior to baseline. Use of a currently marketed drug in a clinical study within 24 weeks prior to baseline would not be exclusionary, provided no other exclusion criteria are met.
  8. Use of immunosuppressive agents, or cytotoxic agents, including cyclophosphamide and azathioprine within 48 weeks prior to baseline.
  9. Previous treatment with fingolimod (GILENYA®, Novartis), dimethyl fumarate (TECFIDERA®, Biogen Idec Inc), glatiramer acetate (COPAXONE®, Teva), interferon-β (either 1a or 1b), intravenous immunoglobulin, or plasmapheresis within 8 weeks prior to baseline.
  10. Use of teriflunomide (AUBAGIO®, Sanofi) within 2 years prior to baseline, except if active washout (with either cholestyramine or activated charcoal) was done 2 months or more prior to baseline.
  11. Prior use of monoclonal antibodies ever, except for:

    1. natalizumab (TYSABRI®, Biogen Idec Inc), if given more than 24 weeks prior to baseline AND the patient is John Cunningham (JC) virus antibody test negative (as per medical history)
    2. rituximab, ocrelizumab, or ofatumumab, if B cell count (CD19, as per medical history) is higher than 80 cells/μL
  12. Use of mitoxantrone (NOVANTRONE®, Immunex) within 5 years prior to screening. Use of mitoxantrone >5 years before screening is allowed in patients with normal ejection fraction and who did not exceed the total lifetime maximal dose.
  13. Previous use of laquinimod.
  14. Chronic (eg, more than 30 consecutive days or monthly dosing, with the intent of MS disease modification) systemic (intravenous, intramuscular or oral) corticosteroid treatment within 8 weeks prior to baseline.
  15. Previous use of cladribine or alemtuzumab (LEMTRADA®, Sanofi).
  16. Previous total body irradiation or total lymphoid irradiation.
  17. Previous stem cell treatment, cell-based treatment, or bone marrow transplantation of any kind.
  18. Patients who underwent endovascular treatment for chronic cerebrospinal venous insufficiency (CCSVI) within 12 weeks prior to baseline.
  19. Use of moderate/strong inhibitors of cytochrome P450 (CYP) 3A4 within 2 weeks prior to baseline.
  20. Use of inducers of CYP3A4 within 2 weeks prior to baseline.
  21. Pregnancy or breastfeeding.
  22. Serum levels ≥3× upper limit of the normal range (ULN) of either alanine aminotransferase (ALT) or aspartate aminotransferase (AST) at screening.
  23. Serum direct bilirubin which is ≥2×ULN at screening.
  24. Patients with a clinically significant or unstable medical or surgical condition that (in the opinion of the Investigator) would preclude safe and complete study participation, as determined by medical history, physical examinations, electrocardiogram (ECG), laboratory tests or chest X-ray.
  25. A known history of hypersensitivity to gadolinium (Gd).
  26. Glomerular filtration rate (GFR) < or equal 60 mL/min at screening visit.
  27. Inability to successfully undergo MRI scanning, including claustrophobia.
  28. Known drug hypersensitivity that would preclude administration of laquinimod, such as hypersensitivity to mannitol, meglumine or sodium stearyl fumarate.

Sites / Locations

  • Teva Investigational Site 12966
  • Teva Investigational Site 12967
  • Teva Investigational Site 12962
  • Teva Investigational Site 12964
  • Teva Investigational Site 12973
  • Teva Investigational Site 12975
  • Teva Investigational Site 12969
  • Teva Investigational Site 12977
  • Teva Investigational Site 13010
  • Teva Investigational Site 12965
  • Teva Investigational Site 12968
  • Teva Investigational Site 12963
  • Teva Investigational Site 12971
  • Teva Investigational Site 12976
  • Teva Investigational Site 12970
  • Teva Investigational Site 11089
  • Teva Investigational Site 11084
  • Teva Investigational Site 11081
  • Teva Investigational Site 11087
  • Teva Investigational Site 11082
  • Teva Investigational Site 11088
  • Teva Investigational Site 32505
  • Teva Investigational Site 32512
  • Teva Investigational Site 32510
  • Teva Investigational Site 32522
  • Teva Investigational Site 32509
  • Teva Investigational Site 32517
  • Teva Investigational Site 32543
  • Teva Investigational Site 32514
  • Teva Investigational Site 32507
  • Teva Investigational Site 32513
  • Teva Investigational Site 32504
  • Teva Investigational Site 32516
  • Teva Investigational Site 32523
  • Teva Investigational Site 32503
  • Teva Investigational Site 32511
  • Teva Investigational Site 30106
  • Teva Investigational Site 30110
  • Teva Investigational Site 30105
  • Teva Investigational Site 30108
  • Teva Investigational Site 30102
  • Teva Investigational Site 30107
  • Teva Investigational Site 30103
  • Teva Investigational Site 30101
  • Teva Investigational Site 30104
  • Teva Investigational Site 38068
  • Teva Investigational Site 38067
  • Teva Investigational Site 38069
  • Teva Investigational Site 53262
  • Teva Investigational Site 53250
  • Teva Investigational Site 53253
  • Teva Investigational Site 53257
  • Teva Investigational Site 53258
  • Teva Investigational Site 53256
  • Teva Investigational Site 53255
  • Teva Investigational Site 53260
  • Teva Investigational Site 53261
  • Teva Investigational Site 53252
  • Teva Investigational Site 50285
  • Teva Investigational Site 50288
  • Teva Investigational Site 50290
  • Teva Investigational Site 50294
  • Teva Investigational Site 50292
  • Teva Investigational Site 50287
  • Teva Investigational Site 50291
  • Teva Investigational Site 50286
  • Teva Investigational Site 50295
  • Teva Investigational Site 50293
  • Teva Investigational Site 50289
  • Teva Investigational Site 31108
  • Teva Investigational Site 31106
  • Teva Investigational Site 31105
  • Teva Investigational Site 31111
  • Teva Investigational Site 31112
  • Teva Investigational Site 31192
  • Teva Investigational Site 31101
  • Teva Investigational Site 31104
  • Teva Investigational Site 31102
  • Teva Investigational Site 31100
  • Teva Investigational Site 58158
  • Teva Investigational Site 58159
  • Teva Investigational Site 58157
  • Teva Investigational Site 58160
  • Teva Investigational Site 58152
  • Teva Investigational Site 58154
  • Teva Investigational Site 58153
  • Teva Investigational Site 58156
  • Teva Investigational Site 58150
  • Teva Investigational Site 58151
  • Teva Investigational Site 34190
  • Teva Investigational Site 34188
  • Teva Investigational Site 34189
  • Teva Investigational Site 34182
  • Teva Investigational Site 34181
  • Teva Investigational Site 34183
  • Teva Investigational Site 34184
  • Teva Investigational Site 34186
  • Teva Investigational Site 34185
  • Teva Investigational Site 34187

Arms of the Study

Arm 1

Arm 2

Arm 3

Arm Type

Placebo Comparator

Experimental

Experimental

Arm Label

Placebo

Laquinimod 0.6 mg

Laquinimod 1.5 mg

Arm Description

once daily oral dose

1 capsule containing 0.6 mg laquinimod and 2 capsules containing placebo were administered orally once daily for at least 48 weeks.

3 capsules containing 0.5 mg laquinimod were administered orally once daily for at least 48 weeks. However this arm was discontinued as of 01 January 2016 and no participants reached the 48 week timeframe.

Outcomes

Primary Outcome Measures

Percent Brain Volume Change (PBVC) From Baseline to Week 48 Using a Repeated Measures ANCOVA Model
Brain atrophy (BA) was measured using magnetic resonance imaging (MRI) scans of the brain. BA was analyzed using baseline-adjusted repeated measures analysis of covariance (ANCOVA- SAS® PROC MIXED) in which 1 contrast was constructed in order to compare between laquinimod 0.6 mg and placebo. The statistical model was a repeated measures analysis of covariance with treatment group, week, treatment group by week interaction, normalized brain volume at baseline, natural logarithm of T2 lesion volume at baseline, and country as fixed effects. Only on-treatment observations (include all the assessments done up to one month after the last dose of the study drug) were included. Values are adjusted means. The cancelled laquinimod 1.5 mg treatment arm was not included in the repeated measures ANCOVA model analysis. However PBVC by visit data are offered in outcome #2.
Percent Brain Volume Change (PBVC) From Baseline to Weeks 24 and 48
Brain atrophy (BA) was measured using magnetic resonance imaging (MRI) scans of the brain. Early termination scans of participants who discontinued the study after week 36 are considered scans at week 48.

Secondary Outcome Measures

Percentage of Participants With 12-Week Confirmed Disability Progression (CDP) As Measured by Expanded Disability Status Scale (EDSS) up to Week 48
CDP was defined as increase in EDSS of >=1 point from baseline EDSS, if EDSS at entry is ≤5.0 or increase of >=0.5 point, if EDSS at entry is >=5.5. This increase should be confirmed after at least 12 weeks. Progression cannot be confirmed during a protocol defined relapse. EDSS is a method of quantifying disability in multiple sclerosis and monitoring changes in the level of disability over time. The EDSS scale ranges from 0 to 10 in 0.5 unit increments with 0=no disability and 10=death due to MS. Only an Examining Neurologist administered the EDSS. The Examining Neurologist did not have access to the patient's medical records or source documents, including previous EDSS forms or adverse events. If a patient died due to MS disease progression, the patient was analyzed as having CDP with the time to CDP as the onset date of progression. If a patient died due to MS before having progression, then the time to disability progression was censored using the date of death.
Percentage of Participants With 12-Week Confirmed Disability Progression (CDP) As Measured by Expanded Disability Status Scale (EDSS) or the Timed 25-foot Walk (T25FW) Test up to Week 48
CDP was defined as increase in EDSS of >=1 point from baseline EDSS, if EDSS at entry is ≤5.0 or increase of >=0.5 point, if EDSS at entry is >=5.5 confirmed after at least 12 weeks, OR increase of >= 20% from baseline in the T25FW test, confirmed after at least 12 weeks. EDSS quantifies disability in MS and monitors changes in the level of disability over time. The EDSS scale is 0-10 in 0.5 unit increments with 0=no disability and 10=death due to MS. The T25-FW is a quantitative mobility and leg function performance test based on the average time of two trials in which participants walk 25 feet as quickly as possible. Increasing time scores indicate increasing impairment. If a patient died due to MS disease progression, the patient was analyzed as having CDP with the time to CDP as the onset date of progression. If a patient died due to MS before having progression, then the time to disability progression was censored using the date of death.
Change From Baseline for the Timed 25-foot Walk (T25FW) Score at Weeks 12, 24, 36 and 48
The T25FW is a quantitative mobility and leg function performance test based on the average time of two trials in which participants walk 25 feet as quickly as possible. In cases when a patient could not complete a T25FW trial due to the physical limitations, a value of 180 seconds was assigned for that trial (this is the maximal possible value for the T25FW test). Increasing time scores indicate increasing impairment. Baseline values are summaries of observed values. Week values are change from baseline values.
Number of New T2 Brain Lesions at Week 48
Inflammatory disease activity was assessed by magnetic resonance imaging (MRI) measurement of the number of new T2 lesions at week 48 as compared to baseline. Scans of patients who discontinued the study after week 36 are considered scans at week 48, and are included in week 48.
Participants With Treatment-Emergent Adverse Events (TEAEs)
An adverse event (AE) was defined as any untoward medical occurrence that develops or worsens in severity during the conduct of a clinical study and does not necessarily have a causal relationship to the study drug. Severity was rated by the investigator on a scale of mild, moderate and severe, with severe= an AE which prevents usual activities. Relationship of AE to treatment was determined by the investigator. Serious AEs include death, a life-threatening adverse event, inpatient hospitalization or prolongation of existing hospitalization, persistent or significant disability or incapacity, a congenital anomaly or birth defect, OR an important medical event that jeopardized the patient and required medical intervention to prevent the previously listed serious outcomes.

Full Information

First Posted
October 31, 2014
Last Updated
March 9, 2022
Sponsor
Teva Branded Pharmaceutical Products R&D, Inc.
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1. Study Identification

Unique Protocol Identification Number
NCT02284568
Brief Title
A Phase 2 Clinical Study in Subjects With Primary Progressive Multiple Sclerosis to Assess the Efficacy, Safety and Tolerability of Two Oral Doses of Laquinimod Either of 0.6 mg/Day or 1.5mg/Day (Experimental Drug) as Compared to Placebo
Acronym
ARPEGGIO
Official Title
A Multinational, Multicenter, Randomized, Double Blind, Parallel Group, Placebo Controlled Study to Evaluate the Efficacy, Safety, and Tolerability of Once Daily Oral Administration of Laquinimod (0.6 or 1.5 mg) in Patients With Primary Progressive Multiple Sclerosis (PPMS)
Study Type
Interventional

2. Study Status

Record Verification Date
March 2022
Overall Recruitment Status
Completed
Study Start Date
January 12, 2015 (Actual)
Primary Completion Date
May 4, 2017 (Actual)
Study Completion Date
October 1, 2017 (Actual)

3. Sponsor/Collaborators

Responsible Party, by Official Title
Sponsor
Name of the Sponsor
Teva Branded Pharmaceutical Products R&D, Inc.

4. Oversight

Studies a U.S. FDA-regulated Drug Product
Yes
Studies a U.S. FDA-regulated Device Product
No
Data Monitoring Committee
Yes

5. Study Description

Brief Summary
This Phase 2 study is intended to serve as a proof of concept for potential treatment with laquinimod in patients with PPMS. The study is also aimed at evaluating 2 doses of laquinimod in this population.
Detailed Description
Due to serious cardiovascular adverse events, Data Monitoring Committee (DMC) made a recommendation to stop all laquinimod treatment arms above 0.6 mg in the multiple sclerosis (MS) trials; therefore the 1.5 mg treatment arm in the ARPEGGIO study was discontinued as of 01 January 2016. The DMC did not identify any definite cardiovascular risk in the 0.6 mg treatment arm, but felt that long term monitoring for emergence of any potential signal was necessary. Therefore, the 0.6 mg treatment arm was continued while the sponsor closely monitored cardiovascular events in all laquinimod studies. Prior to 01 January 2016, eligible patients were randomized in a 1:1:1 ratio into 1 of the following treatment arms (a total of 286 patients were randomized 1:1:1 prior to 01 January 2016): Laquinimod 0.6 mg daily Laquinimod 1.5 mg daily Daily placebo As of 01 January 2016, following the decision to discontinue the laquinimod 1.5 mg dose arm, additional eligible patients (87 patients) who were enrolled were randomized in a 1:1 ratio into one of the following treatment arms: Laquinimod 0.6 mg daily Daily placebo

6. Conditions and Keywords

Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study
Primary Progressive Multiple Sclerosis
Keywords
multiple sclerosis, primary progressive multiple sclerosis, oral immunomodulator

7. Study Design

Primary Purpose
Treatment
Study Phase
Phase 2
Interventional Study Model
Parallel Assignment
Masking
ParticipantCare ProviderInvestigator
Allocation
Randomized
Enrollment
374 (Actual)

8. Arms, Groups, and Interventions

Arm Title
Placebo
Arm Type
Placebo Comparator
Arm Description
once daily oral dose
Arm Title
Laquinimod 0.6 mg
Arm Type
Experimental
Arm Description
1 capsule containing 0.6 mg laquinimod and 2 capsules containing placebo were administered orally once daily for at least 48 weeks.
Arm Title
Laquinimod 1.5 mg
Arm Type
Experimental
Arm Description
3 capsules containing 0.5 mg laquinimod were administered orally once daily for at least 48 weeks. However this arm was discontinued as of 01 January 2016 and no participants reached the 48 week timeframe.
Intervention Type
Drug
Intervention Name(s)
Placebo
Intervention Description
Placebo
Intervention Type
Drug
Intervention Name(s)
Laquinimod
Other Intervention Name(s)
TV-5600
Intervention Description
Laquinimod capsules in 0.5 mg and 0.6 mg strengths
Intervention Type
Drug
Intervention Name(s)
Placebo
Intervention Description
Placebo capsules
Primary Outcome Measure Information:
Title
Percent Brain Volume Change (PBVC) From Baseline to Week 48 Using a Repeated Measures ANCOVA Model
Description
Brain atrophy (BA) was measured using magnetic resonance imaging (MRI) scans of the brain. BA was analyzed using baseline-adjusted repeated measures analysis of covariance (ANCOVA- SAS® PROC MIXED) in which 1 contrast was constructed in order to compare between laquinimod 0.6 mg and placebo. The statistical model was a repeated measures analysis of covariance with treatment group, week, treatment group by week interaction, normalized brain volume at baseline, natural logarithm of T2 lesion volume at baseline, and country as fixed effects. Only on-treatment observations (include all the assessments done up to one month after the last dose of the study drug) were included. Values are adjusted means. The cancelled laquinimod 1.5 mg treatment arm was not included in the repeated measures ANCOVA model analysis. However PBVC by visit data are offered in outcome #2.
Time Frame
Baseline (at least 14 days but not more than 6 weeks prior to Day 1), Weeks 24, 48 and including early termination visits
Title
Percent Brain Volume Change (PBVC) From Baseline to Weeks 24 and 48
Description
Brain atrophy (BA) was measured using magnetic resonance imaging (MRI) scans of the brain. Early termination scans of participants who discontinued the study after week 36 are considered scans at week 48.
Time Frame
Baseline (at least 14 days but not more than 6 weeks prior to Day 1), Weeks 24, 48
Secondary Outcome Measure Information:
Title
Percentage of Participants With 12-Week Confirmed Disability Progression (CDP) As Measured by Expanded Disability Status Scale (EDSS) up to Week 48
Description
CDP was defined as increase in EDSS of >=1 point from baseline EDSS, if EDSS at entry is ≤5.0 or increase of >=0.5 point, if EDSS at entry is >=5.5. This increase should be confirmed after at least 12 weeks. Progression cannot be confirmed during a protocol defined relapse. EDSS is a method of quantifying disability in multiple sclerosis and monitoring changes in the level of disability over time. The EDSS scale ranges from 0 to 10 in 0.5 unit increments with 0=no disability and 10=death due to MS. Only an Examining Neurologist administered the EDSS. The Examining Neurologist did not have access to the patient's medical records or source documents, including previous EDSS forms or adverse events. If a patient died due to MS disease progression, the patient was analyzed as having CDP with the time to CDP as the onset date of progression. If a patient died due to MS before having progression, then the time to disability progression was censored using the date of death.
Time Frame
Baseline (Week 0), Weeks 12, 24, 36, 48 (end if treatment if < 48 weeks)
Title
Percentage of Participants With 12-Week Confirmed Disability Progression (CDP) As Measured by Expanded Disability Status Scale (EDSS) or the Timed 25-foot Walk (T25FW) Test up to Week 48
Description
CDP was defined as increase in EDSS of >=1 point from baseline EDSS, if EDSS at entry is ≤5.0 or increase of >=0.5 point, if EDSS at entry is >=5.5 confirmed after at least 12 weeks, OR increase of >= 20% from baseline in the T25FW test, confirmed after at least 12 weeks. EDSS quantifies disability in MS and monitors changes in the level of disability over time. The EDSS scale is 0-10 in 0.5 unit increments with 0=no disability and 10=death due to MS. The T25-FW is a quantitative mobility and leg function performance test based on the average time of two trials in which participants walk 25 feet as quickly as possible. Increasing time scores indicate increasing impairment. If a patient died due to MS disease progression, the patient was analyzed as having CDP with the time to CDP as the onset date of progression. If a patient died due to MS before having progression, then the time to disability progression was censored using the date of death.
Time Frame
Baseline (Week 0), Weeks 12, 24, 36, 48 (end if treatment if < 48 weeks)
Title
Change From Baseline for the Timed 25-foot Walk (T25FW) Score at Weeks 12, 24, 36 and 48
Description
The T25FW is a quantitative mobility and leg function performance test based on the average time of two trials in which participants walk 25 feet as quickly as possible. In cases when a patient could not complete a T25FW trial due to the physical limitations, a value of 180 seconds was assigned for that trial (this is the maximal possible value for the T25FW test). Increasing time scores indicate increasing impairment. Baseline values are summaries of observed values. Week values are change from baseline values.
Time Frame
Baseline (Week 0), Weeks 12, 24, 36, 48
Title
Number of New T2 Brain Lesions at Week 48
Description
Inflammatory disease activity was assessed by magnetic resonance imaging (MRI) measurement of the number of new T2 lesions at week 48 as compared to baseline. Scans of patients who discontinued the study after week 36 are considered scans at week 48, and are included in week 48.
Time Frame
Baseline (Week 0), 48 weeks
Title
Participants With Treatment-Emergent Adverse Events (TEAEs)
Description
An adverse event (AE) was defined as any untoward medical occurrence that develops or worsens in severity during the conduct of a clinical study and does not necessarily have a causal relationship to the study drug. Severity was rated by the investigator on a scale of mild, moderate and severe, with severe= an AE which prevents usual activities. Relationship of AE to treatment was determined by the investigator. Serious AEs include death, a life-threatening adverse event, inpatient hospitalization or prolongation of existing hospitalization, persistent or significant disability or incapacity, a congenital anomaly or birth defect, OR an important medical event that jeopardized the patient and required medical intervention to prevent the previously listed serious outcomes.
Time Frame
Day 1 up to Week 130 (longest duration of treatment)

10. Eligibility

Sex
All
Minimum Age & Unit of Time
25 Years
Maximum Age & Unit of Time
55 Years
Accepts Healthy Volunteers
No
Eligibility Criteria
Inclusion Criteria: Patients must have a confirmed and documented PPMS diagnosis as defined by the 2010 Revised McDonald criteria Baseline magnetic resonance imaging (MRI) showing lesions consistent with PPMS in either or both brain and spinal cord Patients must have an Expanded Disability Status Scale (EDSS) score of 3 to 6.5, inclusive, at both screening and baseline visits Documented evidence of clinical disability progression in the 2 years prior to screening. Functional System Score (FSS) of > or equal 2 for the pyramidal system or gait impairment due to lower extremity dysfunction Patients must be between 25 to 55 years of age, inclusive Women of child-bearing potential must practice an acceptable method of birth control for 30 days before taking the study drug, and 2 acceptable methods of birth control during all study duration and until 30 days after the last dose of treatment is administered. Patients must sign and date a written informed consent prior to entering the study. Patients must be willing and able to comply with the protocol requirements for the duration of the study. Exclusion Criteria: Patients with history of any multiple sclerosis (MS) exacerbations or relapses, including any episodes of optic neuritis. Progressive neurological disorder other than PPMS. Any MRI record showing presence of cervical cord compression. Baseline MRI showing other findings (including lesions that are atypical for PPMS) that may explain the clinical signs and symptoms. Relevant history of vitamin B12 deficiency. Positive human T-lymphotropic virus Type I and II (HTLV-I/II) serology. Use of experimental or investigational drugs in a clinical study within 24 weeks prior to baseline. Use of a currently marketed drug in a clinical study within 24 weeks prior to baseline would not be exclusionary, provided no other exclusion criteria are met. Use of immunosuppressive agents, or cytotoxic agents, including cyclophosphamide and azathioprine within 48 weeks prior to baseline. Previous treatment with fingolimod (GILENYA®, Novartis), dimethyl fumarate (TECFIDERA®, Biogen Idec Inc), glatiramer acetate (COPAXONE®, Teva), interferon-β (either 1a or 1b), intravenous immunoglobulin, or plasmapheresis within 8 weeks prior to baseline. Use of teriflunomide (AUBAGIO®, Sanofi) within 2 years prior to baseline, except if active washout (with either cholestyramine or activated charcoal) was done 2 months or more prior to baseline. Prior use of monoclonal antibodies ever, except for: natalizumab (TYSABRI®, Biogen Idec Inc), if given more than 24 weeks prior to baseline AND the patient is John Cunningham (JC) virus antibody test negative (as per medical history) rituximab, ocrelizumab, or ofatumumab, if B cell count (CD19, as per medical history) is higher than 80 cells/μL Use of mitoxantrone (NOVANTRONE®, Immunex) within 5 years prior to screening. Use of mitoxantrone >5 years before screening is allowed in patients with normal ejection fraction and who did not exceed the total lifetime maximal dose. Previous use of laquinimod. Chronic (eg, more than 30 consecutive days or monthly dosing, with the intent of MS disease modification) systemic (intravenous, intramuscular or oral) corticosteroid treatment within 8 weeks prior to baseline. Previous use of cladribine or alemtuzumab (LEMTRADA®, Sanofi). Previous total body irradiation or total lymphoid irradiation. Previous stem cell treatment, cell-based treatment, or bone marrow transplantation of any kind. Patients who underwent endovascular treatment for chronic cerebrospinal venous insufficiency (CCSVI) within 12 weeks prior to baseline. Use of moderate/strong inhibitors of cytochrome P450 (CYP) 3A4 within 2 weeks prior to baseline. Use of inducers of CYP3A4 within 2 weeks prior to baseline. Pregnancy or breastfeeding. Serum levels ≥3× upper limit of the normal range (ULN) of either alanine aminotransferase (ALT) or aspartate aminotransferase (AST) at screening. Serum direct bilirubin which is ≥2×ULN at screening. Patients with a clinically significant or unstable medical or surgical condition that (in the opinion of the Investigator) would preclude safe and complete study participation, as determined by medical history, physical examinations, electrocardiogram (ECG), laboratory tests or chest X-ray. A known history of hypersensitivity to gadolinium (Gd). Glomerular filtration rate (GFR) < or equal 60 mL/min at screening visit. Inability to successfully undergo MRI scanning, including claustrophobia. Known drug hypersensitivity that would preclude administration of laquinimod, such as hypersensitivity to mannitol, meglumine or sodium stearyl fumarate.
Overall Study Officials:
First Name & Middle Initial & Last Name & Degree
Teva Medical Expert, MD
Organizational Affiliation
Teva Branded Pharmaceutical Products R&D, Inc.
Official's Role
Study Director
Facility Information:
Facility Name
Teva Investigational Site 12966
City
Phoenix
State/Province
Arizona
ZIP/Postal Code
85018
Country
United States
Facility Name
Teva Investigational Site 12967
City
Newport Beach
State/Province
California
ZIP/Postal Code
92663
Country
United States
Facility Name
Teva Investigational Site 12962
City
San Francisco
State/Province
California
ZIP/Postal Code
94158
Country
United States
Facility Name
Teva Investigational Site 12964
City
Aurora
State/Province
Colorado
ZIP/Postal Code
80045
Country
United States
Facility Name
Teva Investigational Site 12973
City
Northbrook
State/Province
Illinois
ZIP/Postal Code
60062
Country
United States
Facility Name
Teva Investigational Site 12975
City
Kansas City
State/Province
Kansas
ZIP/Postal Code
66160-7314
Country
United States
Facility Name
Teva Investigational Site 12969
City
Lenexa
State/Province
Kansas
ZIP/Postal Code
66214
Country
United States
Facility Name
Teva Investigational Site 12977
City
Golden Valley
State/Province
Minnesota
ZIP/Postal Code
55422
Country
United States
Facility Name
Teva Investigational Site 13010
City
Golden Valley
State/Province
Minnesota
ZIP/Postal Code
55422
Country
United States
Facility Name
Teva Investigational Site 12965
City
Chesterfield
State/Province
Missouri
ZIP/Postal Code
63017
Country
United States
Facility Name
Teva Investigational Site 12968
City
Saint Louis
State/Province
Missouri
ZIP/Postal Code
63110
Country
United States
Facility Name
Teva Investigational Site 12963
City
New York
State/Province
New York
ZIP/Postal Code
10016
Country
United States
Facility Name
Teva Investigational Site 12971
City
Charlotte
State/Province
North Carolina
ZIP/Postal Code
28207
Country
United States
Facility Name
Teva Investigational Site 12976
City
Columbus
State/Province
Ohio
ZIP/Postal Code
43221
Country
United States
Facility Name
Teva Investigational Site 12970
City
Uniontown
State/Province
Ohio
ZIP/Postal Code
44685
Country
United States
Facility Name
Teva Investigational Site 11089
City
Calgary
State/Province
AL
ZIP/Postal Code
T2N 4Z1
Country
Canada
Facility Name
Teva Investigational Site 11084
City
Halifax
State/Province
Nova Scotia
ZIP/Postal Code
B3H 4K4
Country
Canada
Facility Name
Teva Investigational Site 11081
City
Ottawa
State/Province
Ontario
ZIP/Postal Code
K1H 8L6
Country
Canada
Facility Name
Teva Investigational Site 11087
City
Toronto
State/Province
Ontario
ZIP/Postal Code
M5B-1W8
Country
Canada
Facility Name
Teva Investigational Site 11082
City
Montreal
State/Province
Quebec
ZIP/Postal Code
H3A 2B4
Country
Canada
Facility Name
Teva Investigational Site 11088
City
Quebec
ZIP/Postal Code
G1J 1Z4
Country
Canada
Facility Name
Teva Investigational Site 32505
City
Bad Mergentheim
ZIP/Postal Code
97980
Country
Germany
Facility Name
Teva Investigational Site 32512
City
Bamberg
ZIP/Postal Code
96049
Country
Germany
Facility Name
Teva Investigational Site 32510
City
Berlin
ZIP/Postal Code
10117
Country
Germany
Facility Name
Teva Investigational Site 32522
City
Bochum
ZIP/Postal Code
44791
Country
Germany
Facility Name
Teva Investigational Site 32509
City
Dresden
ZIP/Postal Code
01307
Country
Germany
Facility Name
Teva Investigational Site 32517
City
Dusseldorf
ZIP/Postal Code
40225
Country
Germany
Facility Name
Teva Investigational Site 32543
City
Goettigen
ZIP/Postal Code
37075
Country
Germany
Facility Name
Teva Investigational Site 32514
City
Hamburg
ZIP/Postal Code
20099
Country
Germany
Facility Name
Teva Investigational Site 32507
City
Hannover
ZIP/Postal Code
30625
Country
Germany
Facility Name
Teva Investigational Site 32513
City
Munchen
ZIP/Postal Code
81675
Country
Germany
Facility Name
Teva Investigational Site 32504
City
Munchen
ZIP/Postal Code
D-81377
Country
Germany
Facility Name
Teva Investigational Site 32516
City
Rostock
ZIP/Postal Code
18057
Country
Germany
Facility Name
Teva Investigational Site 32523
City
Trier
ZIP/Postal Code
54292
Country
Germany
Facility Name
Teva Investigational Site 32503
City
Ulm
ZIP/Postal Code
89081
Country
Germany
Facility Name
Teva Investigational Site 32511
City
Wurzburg
ZIP/Postal Code
97080
Country
Germany
Facility Name
Teva Investigational Site 30106
City
Cefalu
ZIP/Postal Code
90015
Country
Italy
Facility Name
Teva Investigational Site 30110
City
Firenze
ZIP/Postal Code
50134
Country
Italy
Facility Name
Teva Investigational Site 30105
City
Gallarate
ZIP/Postal Code
21013
Country
Italy
Facility Name
Teva Investigational Site 30108
City
Genova
ZIP/Postal Code
16132
Country
Italy
Facility Name
Teva Investigational Site 30102
City
Milano
ZIP/Postal Code
20127
Country
Italy
Facility Name
Teva Investigational Site 30107
City
Orbassano
ZIP/Postal Code
10043
Country
Italy
Facility Name
Teva Investigational Site 30103
City
Padova
ZIP/Postal Code
35128
Country
Italy
Facility Name
Teva Investigational Site 30101
City
Rome
ZIP/Postal Code
00133
Country
Italy
Facility Name
Teva Investigational Site 30104
City
Rome
ZIP/Postal Code
?00152
Country
Italy
Facility Name
Teva Investigational Site 38068
City
Amsterdam
ZIP/Postal Code
1081 HV
Country
Netherlands
Facility Name
Teva Investigational Site 38067
City
Nijmegen
ZIP/Postal Code
6532 SZ
Country
Netherlands
Facility Name
Teva Investigational Site 38069
City
Sittard
ZIP/Postal Code
6162 BG
Country
Netherlands
Facility Name
Teva Investigational Site 53262
City
Bialystok
ZIP/Postal Code
15-402
Country
Poland
Facility Name
Teva Investigational Site 53250
City
Bydgoszcz
ZIP/Postal Code
85-795
Country
Poland
Facility Name
Teva Investigational Site 53253
City
Gdansk
ZIP/Postal Code
80-803
Country
Poland
Facility Name
Teva Investigational Site 53257
City
Katowice
ZIP/Postal Code
40-635
Country
Poland
Facility Name
Teva Investigational Site 53258
City
Katowice
ZIP/Postal Code
40-684
Country
Poland
Facility Name
Teva Investigational Site 53256
City
Katowice
ZIP/Postal Code
40-749
Country
Poland
Facility Name
Teva Investigational Site 53255
City
Kielce
ZIP/Postal Code
25-726
Country
Poland
Facility Name
Teva Investigational Site 53260
City
Lublin
ZIP/Postal Code
20-954
Country
Poland
Facility Name
Teva Investigational Site 53261
City
Olsztyn
ZIP/Postal Code
10-560
Country
Poland
Facility Name
Teva Investigational Site 53252
City
Warsaw
ZIP/Postal Code
02-957
Country
Poland
Facility Name
Teva Investigational Site 50285
City
Kaluga
ZIP/Postal Code
248007
Country
Russian Federation
Facility Name
Teva Investigational Site 50288
City
Kazan
ZIP/Postal Code
420021
Country
Russian Federation
Facility Name
Teva Investigational Site 50290
City
Kazan
ZIP/Postal Code
420103
Country
Russian Federation
Facility Name
Teva Investigational Site 50294
City
Kirov
ZIP/Postal Code
610006
Country
Russian Federation
Facility Name
Teva Investigational Site 50292
City
Krasnoyarsk
ZIP/Postal Code
660022
Country
Russian Federation
Facility Name
Teva Investigational Site 50287
City
Moscow
ZIP/Postal Code
127018
Country
Russian Federation
Facility Name
Teva Investigational Site 50291
City
Nizhny Novgorod
ZIP/Postal Code
603126
Country
Russian Federation
Facility Name
Teva Investigational Site 50286
City
Novosibirsk
ZIP/Postal Code
630007
Country
Russian Federation
Facility Name
Teva Investigational Site 50295
City
Perm
ZIP/Postal Code
614990
Country
Russian Federation
Facility Name
Teva Investigational Site 50293
City
Saint Petersburg
ZIP/Postal Code
197022
Country
Russian Federation
Facility Name
Teva Investigational Site 50289
City
St. Petersburg
ZIP/Postal Code
194044
Country
Russian Federation
Facility Name
Teva Investigational Site 31108
City
Barcelona
ZIP/Postal Code
08036
Country
Spain
Facility Name
Teva Investigational Site 31106
City
Barcelona
ZIP/Postal Code
8035
Country
Spain
Facility Name
Teva Investigational Site 31105
City
El Palmar
ZIP/Postal Code
30120
Country
Spain
Facility Name
Teva Investigational Site 31111
City
Lleida
ZIP/Postal Code
25198
Country
Spain
Facility Name
Teva Investigational Site 31112
City
Madrid
ZIP/Postal Code
28040
Country
Spain
Facility Name
Teva Investigational Site 31192
City
Madrid
ZIP/Postal Code
28223
Country
Spain
Facility Name
Teva Investigational Site 31101
City
Malaga
ZIP/Postal Code
29010
Country
Spain
Facility Name
Teva Investigational Site 31104
City
San Sebastian
ZIP/Postal Code
20014
Country
Spain
Facility Name
Teva Investigational Site 31102
City
Sevilla
ZIP/Postal Code
41009
Country
Spain
Facility Name
Teva Investigational Site 31100
City
Valencia
ZIP/Postal Code
46026
Country
Spain
Facility Name
Teva Investigational Site 58158
City
Dnipropetrovsk
ZIP/Postal Code
49005
Country
Ukraine
Facility Name
Teva Investigational Site 58159
City
Ivano-Frankivsk
ZIP/Postal Code
76014
Country
Ukraine
Facility Name
Teva Investigational Site 58157
City
Kharkiv
ZIP/Postal Code
61068
Country
Ukraine
Facility Name
Teva Investigational Site 58160
City
Kyiv
ZIP/Postal Code
?03110
Country
Ukraine
Facility Name
Teva Investigational Site 58152
City
Lutsk
ZIP/Postal Code
43005
Country
Ukraine
Facility Name
Teva Investigational Site 58154
City
Lviv
ZIP/Postal Code
79010
Country
Ukraine
Facility Name
Teva Investigational Site 58153
City
Lviv
ZIP/Postal Code
79044
Country
Ukraine
Facility Name
Teva Investigational Site 58156
City
Zaporizhzhia
ZIP/Postal Code
69068
Country
Ukraine
Facility Name
Teva Investigational Site 58150
City
Zaporizhzhya
ZIP/Postal Code
69035
Country
Ukraine
Facility Name
Teva Investigational Site 58151
City
Zaporizhzhya
ZIP/Postal Code
69600
Country
Ukraine
Facility Name
Teva Investigational Site 34190
City
Bristol
ZIP/Postal Code
BS10 5NB
Country
United Kingdom
Facility Name
Teva Investigational Site 34188
City
Edinburgh
ZIP/Postal Code
EH4 2XU
Country
United Kingdom
Facility Name
Teva Investigational Site 34189
City
Exeter
ZIP/Postal Code
EX2 5DW
Country
United Kingdom
Facility Name
Teva Investigational Site 34182
City
Liverpool
ZIP/Postal Code
L9 7LJ
Country
United Kingdom
Facility Name
Teva Investigational Site 34181
City
London
ZIP/Postal Code
E1 2AT
Country
United Kingdom
Facility Name
Teva Investigational Site 34183
City
Nottingham
ZIP/Postal Code
NG7 2UH
Country
United Kingdom
Facility Name
Teva Investigational Site 34184
City
Oxford
ZIP/Postal Code
OX3 9DU
Country
United Kingdom
Facility Name
Teva Investigational Site 34186
City
Plymouth
ZIP/Postal Code
PL6 8DH
Country
United Kingdom
Facility Name
Teva Investigational Site 34185
City
Stoke-on-Trent
ZIP/Postal Code
ST4 6GQ
Country
United Kingdom
Facility Name
Teva Investigational Site 34187
City
Swansea
ZIP/Postal Code
SA6 6NL
Country
United Kingdom

12. IPD Sharing Statement

Citations:
PubMed Identifier
32651286
Citation
Giovannoni G, Knappertz V, Steinerman JR, Tansy AP, Li T, Krieger S, Uccelli A, Uitdehaag BMJ, Montalban X, Hartung HP, Pia Sormani M, Cree BAC, Lublin F, Barkhof F. A randomized, placebo-controlled, phase 2 trial of laquinimod in primary progressive multiple sclerosis. Neurology. 2020 Aug 25;95(8):e1027-e1040. doi: 10.1212/WNL.0000000000010284. Epub 2020 Jul 10.
Results Reference
derived

Learn more about this trial

A Phase 2 Clinical Study in Subjects With Primary Progressive Multiple Sclerosis to Assess the Efficacy, Safety and Tolerability of Two Oral Doses of Laquinimod Either of 0.6 mg/Day or 1.5mg/Day (Experimental Drug) as Compared to Placebo

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