Multiple Sclerosis Clinical Trial
— TOPICOfficial title:
An International, Multi-center, Randomized, Double-blind, Placebo-controlled, Parallel Group Study to Evaluate the Efficacy and Safety of Two Year Treatment With Teriflunomide 7 mg Once Daily and 14 mg Once Daily Versus Placebo in Patients With a First Clinical Episode Suggestive of Multiple Sclerosis Plus a Long Term Extension Period
The primary objective is to demonstrate the effect of teriflunomide (HMR1726) (14 milligram
per day [mg/day] and 7 mg/day), in comparison to placebo, for reducing conversion of
participants presenting with their first clinical episode consistent with multiple sclerosis
(MS) to clinically definite multiple sclerosis (CDMS).
The secondary objectives are:
- To demonstrate the effect of teriflunomide, in comparison to placebo, on:
- Reducing conversion to definite multiple sclerosis (DMS)
- Reducing annualized relapse rate (ARR)
- Reducing disease activity/progression as measured by Magnetic Resonance Imaging
(MRI)
- Reducing accumulation of disability for at least 12 weeks as measured by the
Expanded Disability Status Scale (EDSS)
- Proportion of disability-free participants as assessed by the EDSS
- Reducing participant-reported fatigue
- To evaluate the safety and tolerability of teriflunomide
- To evaluate the pharmacokinetics (PK) of teriflunomide
- Optional pharmacogenomic testing aimed at assessing the association between the main
enzyme systems of teriflunomide metabolism and hepatic safety, and other potential
associations between gene variations and clinical outcomes
| Status | Active, not recruiting |
| Enrollment | 618 |
| Est. completion date | December 2015 |
| Est. primary completion date | December 2012 |
| Accepts healthy volunteers | No |
| Gender | Both |
| Age group | 18 Years to 55 Years |
| Eligibility |
Inclusion Criteria: - First acute or subacute, well-defined neurological event consistent with demyelination (that is, optic neuritis confirmed by an ophthalmologist, spinal cord syndrome, brainstem/cerebellar syndromes) - Onset of MS symptoms occurring within 90 days of randomization - A screening MRI scan with 2 or more T2 lesions at least 3 millimeter (mm) in diameter that are characteristic of MS Exclusion Criteria: - Clinically relevant cardiovascular, hepatic, neurological, endocrine or other major systemic disease - Significantly impaired bone marrow function - Pregnancy or nursing - Alcohol or drug abuse - Use of cladribine, mitoxantrone, or other immunosuppressant agents such as azathioprine, cyclophosphamide, cyclosporin, methotrexate or mycophenolate before enrollment - Any known condition or circumstance that would prevent in the investigator's opinion compliance or completion of the study The above information is not intended to contain all considerations relevant to a participant's potential participation in a clinical trial. |
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Investigator), Primary Purpose: Treatment
| Country | Name | City | State |
|---|---|---|---|
| Australia | Investigational Site Number 1405 | Geelong | |
| Australia | Investigational Site Number 1404 | Heidelberg | |
| Australia | Investigational Site Number 1407 | Hobart | |
| Australia | Investigational Site Number 1401 | Parkville | |
| Austria | Investigational Site Number 4004 | Innsbruck | |
| Austria | Investigational Site Number 4005 | Linz | |
| Austria | Investigational Site Number 4001 | Wien | |
| Bulgaria | Investigational Site Number 5312 | Pleven | |
| Bulgaria | Investigational Site Number 5303 | Sofia | |
| Bulgaria | Investigational Site Number 5304 | Sofia | |
| Bulgaria | Investigational Site Number 5306 | Sofia | |
| Bulgaria | Investigational Site Number 5307 | Sofia | |
| Bulgaria | Investigational Site Number 5309 | Sofia | |
| Canada | Investigational Site Number 5402 | Greenfield Park | |
| Canada | Investigational Site Number 5403 | London | |
| Canada | Investigational Site Number 5409 | Montreal | |
| Canada | Investigational Site Number 5401 | Ottawa | |
| Canada | Investigational Site Number 5406 | Quebec | |
| Canada | Investigational Site Number 5408 | Sherbrooke | |
| Canada | Investigational Site Number 5404 | Toronto | |
| Canada | Investigational Site Number 5410 | Toronto | |
| Chile | Investigational Site Number 5601 | Santiago | |
| Chile | Investigational Site Number 5602 | Santiago | |
| Chile | Investigational Site Number 5606 | Santiago | |
| Chile | Investigational Site Number 5605 | Viña Del Mar | |
| Czech Republic | Investigational Site Number 5801 | Brno | |
| Czech Republic | Investigational Site Number 5803 | Hradec Kralove | |
| Czech Republic | Investigational Site Number 5804 | Olomouc | |
| Czech Republic | Investigational Site Number 5805 | Ostrava - Poruba | |
| Denmark | Investigational Site Number 6002 | Aarhus C | |
| Denmark | Investigational Site Number 6004 | Esbjerg | |
| Estonia | Investigational Site Number 6201 | Tallinn | |
| Estonia | Investigational Site Number 6203 | Tartu | |
| Finland | Investigational Site Number 6405 | Helsinki | |
| Finland | Investigational Site Number 6403 | Kuopio | |
| Finland | Investigational Site Number 6401 | Turku | |
| France | Investigational Site Number 6611 | Besancon | |
| France | Investigational Site Number 6601 | Clermont Ferrand Cedex 1 | |
| France | Investigational Site Number 6609 | Lille Cedex | |
| France | Investigational Site Number 6604 | Montpellier Cedex 05 | |
| France | Investigational Site Number 6612 | Nancy Cedex | |
| France | Investigational Site Number 6605 | Nantes Cedex 01 | |
| France | Investigational Site Number 6602 | Nice Cedex | |
| France | Investigational Site Number 6614 | Nimes | |
| France | Investigational Site Number 6607 | Strasbourg Cedex | |
| Germany | Investigational Site Number 6801 | Bayreuth | |
| Germany | Investigational Site Number 6805 | Berlin | |
| Germany | Investigational Site Number 6810 | Berlin | |
| Germany | Investigational Site Number 6807 | Erbach | |
| Germany | Investigational Site Number 6803 | Essen | |
| Germany | Investigational Site Number 6809 | Hannover | |
| Germany | Investigational Site Number 6804 | Ludwigshafen | |
| Germany | Investigational Site Number 6815 | Minden | |
| Germany | Investigational Site Number 6802 | Münster | |
| Germany | Investigational Site Number 6806 | Wiesbaden | |
| Hungary | Investigational Site Number 7101 | Budapest | |
| Hungary | Investigational Site Number 7103 | Budapest | |
| Hungary | Investigational Site Number 7108 | Esztergom | |
| Hungary | Investigational Site Number 7105 | Veszprém | |
| Lithuania | Investigational Site Number 7402 | Klaipeda | |
| Lithuania | Investigational Site Number 7403 | Siauliai | |
| Lithuania | Investigational Site Number 7401 | Vilnius | |
| Mexico | Investigational Site Number 7501 | Chihuahua | |
| Mexico | Investigational Site Number 7502 | Guadalajara | |
| Poland | Investigational Site Number 7709 | Gdansk | |
| Poland | Investigational Site Number 7710 | Lodz | |
| Poland | Investigational Site Number 7701 | Warszawa | |
| Poland | Investigational Site Number 7703 | Warszawa | |
| Poland | Investigational Site Number 7707 | Warszawa 44 | |
| Romania | Investigational Site Number 7803 | Bucuresti | |
| Romania | Investigational Site Number 7806 | Bucuresti | |
| Romania | Investigational Site Number 7805 | Cluj-Napoca | |
| Romania | Investigational Site Number 7807 | Cluj-Napoca | |
| Romania | Investigational Site Number 7808 | Timisoara | |
| Russian Federation | Investigational Site Number 7907 | Kazan | |
| Russian Federation | Investigational Site Number 7904 | Nizhny Novgorod | |
| Russian Federation | Investigational Site Number 7906 | Nizhny Novgorod | |
| Russian Federation | Investigational Site Number 7909 | Nizhny Novgorod | |
| Russian Federation | Investigational Site Number 7912 | Novosibirsk | |
| Russian Federation | Investigational Site Number 7910 | Rostov-On-Don | |
| Russian Federation | Investigational Site Number 7905 | Smolensk | |
| Russian Federation | Investigational Site Number 7911 | St-Petersburg | |
| Turkey | Investigational Site Number 8304 | Edirne | |
| Turkey | Investigational Site Number 8308 | Istanbul | |
| Turkey | Investigational Site Number 8309 | Istanbul | |
| Turkey | Investigational Site Number 8310 | Istanbul | |
| Turkey | Investigational Site Number 8312 | Istanbul | |
| Turkey | Investigational Site Number 8315 | Istanbul | |
| Turkey | Investigational Site Number 8301 | Izmir | |
| Turkey | Investigational Site Number 8303 | Izmir | |
| Turkey | Investigational Site Number 8305 | Izmir | |
| Turkey | Investigational Site Number 8302 | Izmit | |
| Turkey | Investigational Site Number 8314 | Trabzon | |
| Ukraine | Investigational Site Number 8507 | Chernihiv | |
| Ukraine | Investigational Site Number 8501 | Dnipropetrovsk | |
| Ukraine | Investigational Site Number 8511 | Donets'K | |
| Ukraine | Investigational Site Number 8504 | Kharkiv | |
| Ukraine | Investigational Site Number 8506 | Kharkiv | |
| Ukraine | Investigational Site Number 8508 | Kiev | |
| Ukraine | Investigational Site Number 8512 | Lutsk | |
| Ukraine | Investigational Site Number 8505 | Lviv | |
| Ukraine | Investigational Site Number 8510 | Poltava | |
| Ukraine | Investigational Site Number 8503 | Vinnytsya | |
| Ukraine | Investigational Site Number 8502 | Zaporizhzhya | |
| United Kingdom | Investigational Site Number 8709 | Liverpool | |
| United Kingdom | Investigational Site Number 8701 | London | |
| United Kingdom | Investigational Site Number 8704 | London | |
| United Kingdom | Investigational Site Number 8706 | Newcastle Upon Tyne | |
| United Kingdom | Investigational Site Number 8705 | Nottingham | |
| United Kingdom | Investigational Site Number 8708 | Plymouth | |
| United Kingdom | Investigational Site Number 8707 | Salford | |
| United Kingdom | Investigational Site Number 8702 | Sheffield | |
| United States | Investigational Site Number 8951 | Albuquerque | New Mexico |
| United States | Investigational Site Number 8930 | Burlington | Vermont |
| United States | Investigational Site Number 8941 | Charlotte | North Carolina |
| United States | Investigational Site Number 8965 | Cullman | Alabama |
| United States | Investigational Site Number 8924 | Dayton | Ohio |
| United States | Investigational Site Number 8962 | Fort Collins | Colorado |
| United States | Investigational Site Number 8914 | Ft. Wayne | Indiana |
| United States | Investigational Site Number 8955 | Grand Rapids | Michigan |
| United States | Investigational Site Number 8940 | Indianapolis | Indiana |
| United States | Investigational Site Number 8920 | Maitland | Florida |
| United States | Investigational Site Number 8925 | New York | New York |
| United States | Investigational Site Number 8946 | Phoenix | Arizona |
| United States | Investigational Site Number 8954 | Phoenix | Arizona |
| United States | Investigational Site Number 8905 | Round Rock | Tennessee |
| United States | Investigational Site Number 8963 | Seattle | Washington |
| United States | Investigational Site Number 8922 | Shreveport | Louisiana |
| United States | Investigational Site Number 8937 | St Louis | Missouri |
| United States | Investigational Site Number 8953 | St. Petersburg | Florida |
| United States | Investigational Site Number 8949 | Traverse City | Michigan |
| Lead Sponsor | Collaborator |
|---|---|
| Sanofi |
United States, Australia, Austria, Bulgaria, Canada, Chile, Czech Republic, Denmark, Estonia, Finland, France, Germany, Hungary, Lithuania, Mexico, Poland, Romania, Russian Federation, Turkey, Ukraine, United Kingdom,
| Type | Measure | Description | Time frame | Safety issue |
|---|---|---|---|---|
| Other | Liver Function: Number of Participants With Potentially Clinically Significant Abnormalities (PCSA) | PCSA values are abnormal values considered medically important by the Sponsor according to predefined criteria based on literature review. Hepatic parameters thresholds were defined as follows: Alanine Aminotransferase (ALT) >3, 5, 10 or 20 upper limit of normal(ULN); Aspartate aminotransferase (AST) >3, 5, 10 or 20 ULN; Alkaline Phosphatase >1.5 ULN; Total Bilirubin (TB) >1.5, 2, or 3 ULN; ALT >3 ULN and TB >2 ULN. |
From first study drug intake up to 112 days after last intake in the placebo-controlled period or up to first intake in the extension treatment period, whichever occurred first | Yes |
| Primary | Time to Conversion to Clinically De?nite Multiple Sclerosis (CDMS) | Conversion to CDMS was defined by the occurrence of a relapse, which was defined as a new neurological abnormality separated by at least 30 days from onset of a preceding clinical event, presented for at least 24 hours and occurred in the absence of fever or known infection. Percent probability of conversion at 24, 48, and 108 weeks was estimated using Kaplan-Meier method. | Up to a maximum of 108 weeks depending on time of enrollment | No |
| Secondary | Time to Conversion to Definite Multiple Sclerosis (DMS) | Conversion to DMS was demonstrated by dissemination of MRI lesions in time (as per McDonald criteria) or a relapse, whichever occurs first. MRI Imaging criteria were detection of Gadolinium (Gd) enhancement at least 3 months after onset of initial clinical event, if not at site corresponding to initial event; detection of new T2 lesion if it appears at any time compared with reference scan (done at time of screening) done at least 30 days after onset of the initial clinical event. Occurrence of relapse was defined as new neurological abnormality separated by at least 30 days from onset of preceding clinical event, present for at least 24 hours and occurring in absence of fever or known infection. New clinical abnormality (neurological sign) that is consistent with participant's symptoms with increase in at least one Functional System (FS) or EDSS score compared to last EDSS assessment. Percent probability of conversion at 24, 48, and 108 weeks was estimated using Kaplan-Meier method. | Up to a maximum of 108 weeks depending on time of enrollment | No |
| Secondary | Annualized Relapse Rate (ARR) | ARR is the total number of confirmed relapses that occurred during the treatment period divided by the total number of patient-years treated. Each episode of relapse (appearance, or worsening of a clinical symptom that was stable for at least 30 days, that persisted for a minimum of 24 hours in the absence of fever) was to be confirmed by an increase in EDSS score or Functional System scores. ARR was assessed using Poisson regression model with robust error variance. To account for the different treatment durations among participants, a Poisson regression model with robust error variance was used (total number of confirmed relapses onset between randomization date and last dose date as the response variable, treatment, region and baseline monofocal/multifocal status as covariates, and log-transformed treatment duration as an offset variable). | Up to a maximum of 108 weeks depending on time of enrollment | No |
| Secondary | Brain Magnetic Resonance Imaging (MRI) Assessment: Change From Baseline in Total Lesion Volume at Week 108 | The total lesion volume (burden of disease) is the total volumes of hyperintense on T2 plus hypointense on T1 as measured by MRI scan. Least-square means were estimated using a Mixed-effect model with repeated measures (MMRM) on cubic root transformed volume data with factors for treatment, baseline monofocal/multifocal status, region, visit, treatment-by-visit interaction, cubic root transformed baseline burden of disease, and baseline-by-visit interaction. | Baseline, Week 108 | No |
| Secondary | Brain MRI Assessment: Number of Gadolinium Enhancing (Gd-enhancing) T1-lesions Per MRI Scan (Poisson Regression Estimates) | Number of Gd-enhancing T1-lesions per scan is the total number of Gd-enhancing T1-lesions that occurred during the treatment period divided by the total number of scans performed during the treatment period. To account for the different numbers of scans performed among the participants, a Poisson regression model with robust error variance was used (total number of Gd-enhancing T1-lesions as response variable, treatment, baseline monofocal/multifocal status, region and baseline number of Gd-enhancing T1-lesions as covariates, and log-transformed number of scans as an offset variable). | Up to a maximum of 108 weeks depending on time of enrollment | No |
| Secondary | Brain MRI Assessment: Volume of Gadolinium Enhancing (Gd-enhancing) T1-lesions Per MRI Scan | Total volume of Gd-enhancing T1-lesions per scan is the sum of the volumes of Gd-enhancing T1-lesions observed during the treatment period divided by the total number of scans performed during the treatment period. To account for the different numbers of scans performed among the participants, a Poisson regression model with robust error variance was used (total number of Gd-enhancing T1-lesions as response variable, treatment, baseline monofocal/multifocal status, region and baseline number of Gd-enhancing T1-lesions as covariates, and log-transformed number of scans as an offset variable). | Up to a maximum of 108 weeks depending on time of enrollment | No |
| Secondary | Brain MRI Assessment: Change From Baseline in Volume of Hypointense Post-Gadolinium T1 Lesion Component | Volume of hypointense post-gadolinium T1 lesion component was measured by MRI scan. Least-square means were estimated using a Mixed-effect model with repeated measures (MMRM) on cubic root transformed volume data adjusted for baseline monofocal/multifocal status, region, visit, treatment-by-visit interaction, cubic root transformed baseline value, and baseline-by-visit interaction | Baseline, Week 108 | No |
| Secondary | Brain MRI Assessment: Change From Baseline in Volume of T2 Lesion Component | Volume of T2 lesion component was measured by MRI scan. Least-square means were estimated using a Mixed-effect model with repeated measures (MMRM) on cubic root transformed volume data adjusted for baseline monofocal/multifocal status, region, visit, treatment-by-visit interaction, cubic root transformed baseline value, and baseline-by-visit interaction. | Baseline, Week 108 | Yes |
| Secondary | Brain MRI Assessment: Percent Change From Baseline in Atrophy | Atrophy was measured by MRI scan. | Baseline, Week 108 | No |
| Secondary | Time to 12-Week Sustained Disability Progression | The 12-week sustained disability progression was defined as increase from baseline of at least 1-point in EDSS score (at least 0.5-point for participants with baseline EDSS score of greater than [>] 5.5) that persisted for at least 12 weeks. Percent probability of participants free of 12-week sustained disability progression at 24, 48, and 108 weeks was estimated using Kaplan-Meier method. | Up to a maximum of 108 weeks depending on time of enrollment | No |
| Secondary | Change From Baseline in EDSS at Week 108 | EDSS is an ordinal scale in half-point increments that qualifies disability in participants with MS. It consists of 8 ordinal rating scales assessing seven functional systems (visual, brainstem, pyramidal, cerebellar, sensory, bowel/bladder and cerebral) as well as ambulation. EDSS total score ranges from 0 (normal neurological examination) to 10 (death due to MS). Least-square means were estimated using a Mixed-effect model with repeated measures (MMRM) on cubic root transformed volume data adjusted for baseline monofocal/multifocal status, region, visit, treatment-by-visit interaction, baseline value and baseline-by-visit interaction | Baseline, Week 108 | No |
| Secondary | Change From Baseline in Fatigue Impact Scale (FIS) Total Score at Week 108 | FIS is a participant-reported scale that qualifies the impact of fatigue on daily life in participants with MS. It consists of 40 statements that measure fatigue in three areas; physical, cognitive, and social. FIS total score ranges from 0 (no problem) to 160 (extreme problem). Least-square means were estimated using a Mixed-effect model with repeated measures [MMRM] on FIS total score data adjusted for or baseline monofocal/multifocal status, region, visit, treatment-by-visit interaction, baseline value and baseline-by-visit interaction. | Baseline, Week 108 | No |
| Secondary | Overview of Adverse Events (AEs) | AEs are any unfavorable and unintended sign, symptom, syndrome, or illness observed by the investigator or reported by the participant during the study. | From first study drug intake up to 112 days after last intake in the placebo-controlled period or up to first intake in the extension treatment period, whichever occurred first | Yes |
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