Relapsing Forms of Multiple Sclerosis (RMS) Study of Bruton's Tyrosine Kinase (BTK) Inhibitor Tolebrutinib (SAR442168) (GEMINI 2)

Recruitment Status
COMPLETED - HAS RESULTS
(See Contacts and Locations)Verified May 2025 by Sanofi
Sponsor
Sanofi
Information Provided by (Responsible Party)
Sanofi
Clinicaltrials.gov Identifier
NCT04410991
Other Study ID Numbers:
EFC16034
First Submitted
May 27, 2020
First Posted
May 31, 2020
Results First Posted
June 2, 2025
Last Update Posted
July 1, 2025
Last Verified
May 2025

ClinicalTrials.gov processed this data on June 2025Link to the current ClinicalTrials.gov record .

History of Changes

Study Details

Study Description

Study duration varied per participant in this event driven trial with a treatment duration of approximately 18 to 36 months. Participants completing the study were offered to participate in a long term safety study.

Condition or DiseaseIntervention/Treatment
Relapsing Multiple Sclerosis
Drug: TolebrutinibDrug: Teriflunomide HMR1726

Study Design

Study TypeInterventional
Actual Enrollment899 participants
Design AllocationRandomized
Interventional ModelParallel Assignment
MaskingTriple
Primary PurposeTreatment
Official TitleA Phase 3, Randomized, Double-blind Efficacy and Safety Study Comparing SAR442168 to Teriflunomide (Aubagio®) in Participants With Relapsing Forms of Multiple Sclerosis
Study Start DateJune 10, 2020
Actual Primary Completion DateJuly 15, 2024
Actual Study Completion DateJuly 15, 2024

Groups and Cohorts

Group/CohortIntervention/Treatment
SAR442168
Dose 1 of oral SAR442168 daily + placebo to match the teriflunomide tablet once daily
Drug: Tolebrutinib
Pharmaceutical form: Tablet Route of administration: Oral
Teriflunomide
Oral 14 mg oral teriflunomide + placebo to match the SAR442168 tablet once daily
Drug: Teriflunomide HMR1726
Pharmaceutical form: Tablet Route of administration: Oral

Outcome Measures

Primary Outcome Measures
  1. Annualized Relapse Rate (ARR) as Assessed by Confirmed Protocol-defined Adjudicated Relapses
    Multiple sclerosis (MS) relapse was defined as a monophasic, acute or subacute onset of new neurological symptoms or worsening of previous neurological symptoms with an objective change on neurological examination. Symptoms were attributable to MS, lasted for \>=24 hours with or without recovery, present at normal body temperature, and preceded by \>=30 days of clinical stability.
Secondary Outcome Measures
  1. Time to Onset of 6-Month Confirmed Disability Worsening as Assessed by Expanded Disability Status Scale
    The EDSS was a disability scale that assessed the following 7 functional domains: visual, brainstem, pyramidal \[motor\], cerebellar \[coordination\], sensory, cerebral, and bowel/bladder. The total EDSS score ranged from 0 (normal) to 10 (death due to MS), increasing in increments of 0.5 points. Higher scores indicated increased disability. Time to onset of 6-month CDW was defined as the time from randomization to the onset of a confirmed, sustained increase from baseline in EDSS score (of \>=1.5 points when the baseline score was 0, of \>=1.0 point when the baseline score was 0.5 to \<=5.5, of \>=0.5 points when the baseline EDSS score was \>5.5) over at least 6 months that was not attributable to another etiology.
  2. Time to Onset of 3-Month Confirmed Disability Worsening as Assessed by Expanded Disability Status Scale
    The EDSS was a disability scale that assessed the following 7 functional domains: visual, brainstem, pyramidal \[motor\], cerebellar \[coordination\], sensory, cerebral, and bowel/bladder. The total EDSS score ranged from 0 (normal) to 10 (death due to MS), increasing in increments of 0.5 points. Higher scores indicated increased disability. Time to onset of 3-month CDW was defined as the time from randomization to the onset of a confirmed, sustained increase from baseline in EDSS score (of \>=1.5 points when the baseline score was 0, of \>=1.0 point when the baseline score was 0.5 to \<=5.5, of \>=0.5 points when the baseline EDSS score was \>5.5) over at least 3 months that was not attributable to another etiology.
  3. Mean Number of New and/or Enlarging T2-Hyperintense Lesions Per Year
    Magnetic resonance imaging (MRI) of the brain was performed to identify number of new and/or enlarging T2-hyperintense lesions defined as the sum of the individual number of new and/or enlarging T2 lesions starting from baseline up to and including the EOS visit.
  4. Mean Number of New Gadolinium-Enhancing T1-Hyperintense Lesions Per Scan
    MRI of the brain was performed to identify number of new Gd-enhancing T1-hyperintense lesions defined as the sum of the individual number of new Gd- enhancing T1-hyperintense lesions starting from baseline up to and including the EOS visit.
  5. Change From Baseline in Cognitive Function as Assessed by the Symbol Digit Modalities Test (SDMT) at EOS
    The SDMT was used to assess processing speed, divided attention, visual scanning, tracking and motor speed. It involved a simple substitution task using a reference key. The number of correct substitutions and number of items completed within a 90 second interval (maximum 110 seconds) were recorded. A decrease of 4 points from baseline on the SDMT was considered meaningful worsening. The score was the number of correctly coded items from 0-110 in 90 seconds; higher scores indicating a better outcome. Baseline was defined as the last available value prior to the first dose of study intervention.
  6. Change From Baseline in Cognitive Function as Assessed by the California Verbal Learning Test Second Edition (CVLT-II) at EOS
    The CVLT-II was a verbal learning and memory test consisting of recall and recognition of a list of 16 words. For each assessment, 5 trials were completed. Total Correct Recall Trials 1-5 was scaled to a normalized T-score metric, which had a mean of 50 and standard deviation of 10, the maximum possible score was 80 and a minimum was 0. Higher values indicated improved cognitive function. Baseline was defined as the last available value prior to the first dose of study intervention.
  7. Time to Onset of 6-Month Confirmed Disability Improvement (CDI) as Assessed by Expanded Disability Status Scale
    The EDSS was a disability scale that assessed the following 7 functional domains: visual, brainstem, pyramidal \[motor\], cerebellar \[coordination\], sensory, cerebral, and bowel/bladder. The total EDSS score ranged from 0 (normal) to 10 (death due to MS), increasing in increments of 0.5 points. Higher scores indicated increased disability. CDI was defined as a decrease of \>=1 point from baseline in the EDSS score lasting at least 6 months.
  8. Percent Change in Brain Volume Loss at EOS Compared to Month 6
    MRI of the brain was performed at the specified timepoints to detect the changes in brain volume loss.
  9. Change From Baseline in Multiple Sclerosis Quality of Life 54 (MSQoL-54) Questionnaire Score at EOS
    MSQoL-54 was standardized instrument comprising generic and MS-specific items. This 54-item instrument generated 12 subscales and 2 single-item measures (satisfaction with sexual function \[1 item\]; change in health \[1 item\]). 12 subscales were: a: physical health (10 items), b: health perceptions (5 items), c: energy (5 items), d: role limit physical (4 items), e: sexual function (4 items), f: pain (3 items), g: social function (3 items), h: health distress (4 items), i: overall quality of life (2 items), j: emotional well-being (5 items), k: role limitations emotional (3 items) and l: cognitive function (4 items). Physical and mental health composite score were calculated as weighted sum of 'a to h' and 'i to l' subscales respectively. Each composite score was transformed linearly to common 0 (worst) to 100 (best) score range; higher score indicated improved quality of life. Baseline was defined as last available value prior to first dose of study intervention.
  10. Number of Participants With Treatment-emergent Adverse Events (TEAEs), Treatment-emergent Serious Adverse Events (TESAEs), TEAEs Leading to Permanent Study Intervention Discontinuation and Adverse Events of Special Interest (AESIs)
    An AE was any untoward medical occurrence in a participant or clinical study participant, temporally associated with the use of study intervention, whether or not considered related to the study intervention. SAE was any untoward medical occurrence that at any dose: resulted in death, was life-threatening, required inpatient hospitalization or prolongation of existing hospitalization, resulted in persistent disability/incapacity, was a congenital anomaly/birth defect or was an important medical event. An AESI was an AE (serious or nonserious) of scientific and medical concern specific to the Sponsor's product or program for which ongoing monitoring and immediate notification by the Investigator to the Sponsor was required. TEAEs were defined as AEs that developed, worsened or became serious during the treatment period.
  11. Change From Baseline in Plasma Neurofilament Light Chain (NfL) and Serum Chitinase-3 Like Protein-1 (Chi3L1) Levels at EOS
    Blood samples were collected at specified timepoints to assess change from baseline in NfL and Chi3L1. Baseline was defined as the last available value prior to the first dose of study intervention.
  12. Change From Baseline in Serum Immunoglobulin (Ig) Levels at EOS
    Blood samples were collected at specified timepoints to assess change from baseline in IgG and IgM levels. Baseline was defined as the last available value prior to the first dose of study intervention.

Eligibility Criteria

Ages Eligible for Study(Adult)
Sexes Eligible for StudyAll
Accepts Healthy VolunteersNo
Inclusion Criteria
Inclusion criteria :
The participant must be 18 to 55 years of age, inclusive, at the time of signing the informed consent
The participant must have been diagnosed with RMS according to the 2017 revision of the McDonald diagnostic criteria
The participant has an expanded disability status scale (EDSS) score ≤5.5 at the first Screening Visit
The participant must have at least 1 of the following prior to screening:
≥1 documented relapse within the previous year OR
≥2 documented relapses within the previous 2 years, OR
≥1 documented Gd enhancing lesion on an MRI scan within the previous year
Contraceptive use by men or women should be consistent with local regulations regarding the methods of contraception for those participating in clinical studies
Male participants are eligible to participate if they agree to the following during the intervention period and until accelerated elimination procedure:
Refrain from donating sperm Plus either:
Be abstinent from heterosexual intercourse as their preferred and usual lifestyle (abstinent on a long term and persistent basis) and agree to remain abstinent OR
Must agree to use contraception/barrier as detailed below
Agree to use a male condom and should also be advised of the benefit for a female partner to use a highly effective method of contraception as a condom may break or leak when having sexual intercourse with a woman of childbearing potential (WOCBP) who is not currently pregnant \- A female participant is eligible to participate if she is not pregnant or breastfeeding, and at least one of the following conditions apply:
Is not a WOCBP OR
Is a WOCBP and agrees to use a contraceptive method that is highly effective (with a failure rate of \<1% per year), preferably with low user dependency during the intervention period and until accelerated elimination procedure is completed (or for at least 10 days after the last dose of SAR442168, if the case was unblinded) and agrees not to donate eggs (ova, oocytes) for the purpose of reproduction during the study and for the same period of time.
A WOCBP must have a negative highly sensitive pregnancy test at screening and within 24hours before the first dose of study intervention.
If a urine test cannot be confirmed as negative (eg, an ambiguous result), a serum pregnancy test is required. In such cases, the participant must be excluded from participation if the serum pregnancy result is positive.
The Investigator is responsible for review of medical history, menstrual history, and recent sexual activity to decrease the risk for inclusion of a woman with an early undetected pregnancy.
The participant must have given written informed consent prior to undertaking any study related procedure. This includes consent to comply with the requirements and restrictions listed in the informed consent form (ICF) and in this protocol. In countries where the legal age of maturity is greater than 18 years, a specific ICF for such legally minor participants must also be signed by the participant's legally authorized representative
Exclusion Criteria
Inclusion criteria :
The participant must be 18 to 55 years of age, inclusive, at the time of signing the informed consent
The participant must have been diagnosed with RMS according to the 2017 revision of the McDonald diagnostic criteria
The participant has an expanded disability status scale (EDSS) score ≤5.5 at the first Screening Visit
The participant must have at least 1 of the following prior to screening:
≥1 documented relapse within the previous year OR
≥2 documented relapses within the previous 2 years, OR
≥1 documented Gd enhancing lesion on an MRI scan within the previous year
Contraceptive use by men or women should be consistent with local regulations regarding the methods of contraception for those participating in clinical studies
Male participants are eligible to participate if they agree to the following during the intervention period and until accelerated elimination procedure:
Refrain from donating sperm Plus either:
Be abstinent from heterosexual intercourse as their preferred and usual lifestyle (abstinent on a long term and persistent basis) and agree to remain abstinent OR
Must agree to use contraception/barrier as detailed below
Agree to use a male condom and should also be advised of the benefit for a female partner to use a highly effective method of contraception as a condom may break or leak when having sexual intercourse with a woman of childbearing potential (WOCBP) who is not currently pregnant \- A female participant is eligible to participate if she is not pregnant or breastfeeding, and at least one of the following conditions apply:
Is not a WOCBP OR
Is a WOCBP and agrees to use a contraceptive method that is highly effective (with a failure rate of \<1% per year), preferably with low user dependency during the intervention period and until accelerated elimination procedure is completed (or for at least 10 days after the last dose of SAR442168, if the case was unblinded) and agrees not to donate eggs (ova, oocytes) for the purpose of reproduction during the study and for the same period of time.
A WOCBP must have a negative highly sensitive pregnancy test at screening and within 24hours before the first dose of study intervention.
If a urine test cannot be confirmed as negative (eg, an ambiguous result), a serum pregnancy test is required. In such cases, the participant must be excluded from participation if the serum pregnancy result is positive.
The Investigator is responsible for review of medical history, menstrual history, and recent sexual activity to decrease the risk for inclusion of a woman with an early undetected pregnancy.
The participant must have given written informed consent prior to undertaking any study related procedure. This includes consent to comply with the requirements and restrictions listed in the informed consent form (ICF) and in this protocol. In countries where the legal age of maturity is greater than 18 years, a specific ICF for such legally minor participants must also be signed by the participant's legally authorized representative Exclusion criteria:
The participant has been diagnosed with primary progressive multiplesclerosis (PPMS) according to the 2017 revision of the McDonald diagnostic criteria or with nonrelapsing secondary progressive multiplesclerosis (SPMS)
The participant has a history of infection or may be at risk for infection including but not limited to: HIV, transplantation, live attenuated vaccines, progressive multifocal leukoencephalopathy, tuberculosis, hepatitis B or C, any persistent chronic or active recurring infection
Clinically significant laboratory abnormalities (including evidence of liver injury) or electrocardiogram abnormalities at Screening.
The participant has conditions or situations that would adversely affect participation in this study, including but not limited to:
A short life expectancy due to pre-existing health condition(s) as determined by their treating neurologist
Medical condition(s) or concomitant disease(s) making them nonevaluable for the primary efficacy endpoint or that would adversely affect participation in this study, as judged by the Investigator
A requirement for concomitant treatment that could bias the primary evaluation
The participant has a history of or currently has concomitant medical or clinical conditions that would adversely affect participation in this study
At screening, the participant is positive for hepatitis B surface antigen and/or hepatitis B core antibody and/or is positive for hepatitis C antibody
The participant has any of the following:
A bleeding disorder or known platelet dysfunction at any time prior to the screening visit
A platelet count \<150 000/μL at the screening visit
The participant has a lymphocyte count below the lower limit of normal (LLN) at the screening visit
The presence of psychiatric disturbance or substance abuse
Prior/concomitant therapy
The participant is receiving potent and moderate inducers of cytochrome P450 (CYP) 3A or potent inhibitors of CYP2C8 hepatic enzymes
The participant is receiving anticoagulant/antiplatelet therapies
The above information is not intended to contain all considerations relevant to a patient's potential participation in a clinical trial

Contacts and Locations

Sponsors and CollaboratorsSanofi
Locations
North Central Neurology Associates, PC-Site Number:8400009 | Cullman Alabama, United States, 35058Center for Neurology and Spine-Site Number:8400089 | Phoenix Arizona, United States, 84018Arcadia Neurology Center-Site Number:8400070 | Arcadia California, United States, 91006Multiple Sclerosis Center of California-Site Number:8400135 | Newport Beach California, United States, 92663Harbor UCLA-Site Number:8400088 | Torrance California, United States, 90502Mountain Neurological Research Center, Inc.-Site Number:8400128 | Basalt Colorado, United States, 81621Advanced Neurosciences Research-Site Number:8400025 | Fort Collins Colorado, United States, 80528South Florida Neurology Associates-Site Number:8400029 | Boca Raton Florida, United States, 33487University of Florida Health-Site Number:8400159 | Gainesville Florida, United States, 32608Neurology Associates, PA-Site Number:8400004 | Maitland Florida, United States, 32761University of Miami-Site Number:8400063 | Miami Florida, United States, 33136Infinity Clinical Research-Site Number:8400008 | Sunrise Florida, United States, 33351University of South Florida-Site Number:8400006 | Tampa Florida, United States, 33612Meridian Clinical Research-Site Number:8400003 | Savannah Georgia, United States, 31406Consultants In Neurology-Site Number:8400011 | Northbrook Illinois, United States, 60062Prairie Education and Research Cooperative-Site Number:8400071 | Springfield Illinois, United States, 62701Fort Wayne Neurological Center-Site Number:8400039 | Fort Wayne Indiana, United States, 46804CHI Saint Joseph Medical Group Neurology-Site Number:8400110 | Lexington Kentucky, United States, 40509University of Kentucky-Site Number:8400106 | Lexington Kentucky, United States, 40536Norton Neurology MS Services-Site Number:8400127 | Louisville Kentucky, United States, 40207The NeuroMedical Center-Site Number:8400057 | Baton Rouge Louisiana, United States, 70810International Neurorehabilitation Institute-Site Number:8400034 | Lutherville-Timonium Maryland, United States, 21093Wayne State University-Site Number:8400046 | Detroit Michigan, United States, 48201Minneapolis Clinic of Neurology-Site Number:8400051 | Minneapolis Minnesota, United States, 55422Saint Luke's Hospital-Site Number:8400153 | Kansas City Missouri, United States, 64111West Omaha Family Physicians-Site Number:8400139 | Omaha Nebraska, United States, 68130University Of Nebraska-Site Number:8400129 | Omaha Nebraska, United States, 68198Hackensack University Hospital-Site Number:8400047 | Hackensack New Jersey, United States, 07601University of New Mexico-Site Number:8400032 | Albuquerque New Mexico, United States, 87131South Shore Neurologic Associates-Site Number:8400100 | Patchogue New York, United States, 11772Novant Health Multiple Sclerosis Care Center - South Park-Site Number:8400120 | Charlotte North Carolina, United States, 28210Meridian Clinical Research, LLC-Site Number:8400005 | Raleigh North Carolina, United States, 27607Sanford Brain & Spine Center-Site Number:8400126 | Fargo North Dakota, United States, 58103Dayton Center for Neurological Disorders-Site Number:8400081 | Centerville Ohio, United States, 45459Jefferson Neurology Associates-Site Number:8400016 | Philadelphia Pennsylvania, United States, 19107Premier Neurology-Site Number:8400069 | Greer South Carolina, United States, 29650Advanced Neuroscience Center-Site Number:8400035 | Franklin Tennessee, United States, 37064Sibyl Wray, MD, Neurology, PC-Site Number:8400007 | Knoxville Tennessee, United States, 37922Mt Olympus Medical Research-Site Number:8400163 | Katy Texas, United States, 77450Neurology Center of San Antonio-Site Number:8400036 | San Antonio Texas, United States, 78258Texas Institute for Neuroogical Disorders-Sherman-Site Number:8400151 | Sherman Texas, United States, 75092Neurological Associates-Site Number:8400097 | Richmond Virginia, United States, 23229Wheaton Franciscan Healthcare-Site Number:8400022 | Milwaukee Wisconsin, United States, 53215Investigational Site Number :0320004 | CABA Buenos Aires, Argentina, C1023AABInvestigational Site Number :0320002 | Capital Federal Buenos Aires, Argentina, 1012Investigational Site Number :0320001 | CABA Buenos Aires F.D., Argentina, C1061Investigational Site Number :0320003 | Rosario Santa Fe Province, Argentina, 2000Investigational Site Number :0320005 | San Miguel de Tucumán , Argentina, T4000AXLInvestigational Site Number :0560005 | Bruges , Belgium, B-8000Investigational Site Number :0560004 | Ghent , Belgium, 9000Investigational Site Number :0560002 | Mons , Belgium, 7000Investigational Site Number :0560001 | Overpelt , Belgium, 3900Investigational Site Number :0760001 | Porto Alegre Rio Grande do Sul, Brazil, 90610-000Investigational Site Number :0760002 | Curitiba , Brazil, 81210-310Investigational Site Number :0760007 | São Paulo , Brazil, 01228-000Investigational Site Number :1240002 | Edmonton Alberta, Canada, T6G 2C8Investigational Site Number : 1240012 | Hamilton Ontario, Canada, L8L 2X2Investigational Site Number :1240014 | London Ontario, Canada, N6A 5A5Investigational Site Number :1240005 | Greenfield Park Quebec, Canada, J4V 2J2Investigational Site Number :1240006 | Gatineau , Canada, J8Y1W2Investigational Site Number :1240021 | Québec , Canada, G1W 4R4Investigational Site Number :1520002 | Santiago Reg Metropolitana de Santiago, Chile, 7650568Investigational Site Number :1520005 | Santiago Reg Metropolitana de Santiago, Chile, 833-0024Investigational Site Number :1520001 | Santiago Reg Metropolitana de Santiago, Chile, 8380456Investigational Site Number :1520003 | Santiago Reg Metropolitana de Santiago, Chile, 8431657Investigational Site Number :1520006 | Concepción , Chile, Investigational Site Number :1520004 | Valdivia , Chile, 5110683Investigational Site Number :1910001 | Zagreb , Croatia, 10000Investigational Site Number :1910002 | Zagreb , Croatia, 10000Investigational Site Number :1910003 | Zagreb , Croatia, 10000Investigational Site Number :2030002 | Brno , Czechia, 65691Investigational Site Number :2030011 | Hradec Králové , Czechia, 50005Investigational Site Number :2030001 | Jihlava , Czechia, 58633Investigational Site Number :2030008 | Prague , Czechia, 10034Investigational Site Number :2030005 | Praha 5 - Motol , Czechia, 15006Investigational Site Number :2500019 | Besançon , France, 25000Investigational Site Number :2500018 | Bordeaux , France, Investigational Site Number :2500011 | Bron , France, 69500Investigational Site Number :2500005 | Clermont-Ferrand , France, 63003Investigational Site Number :2500006 | Montpellier , France, 34295Investigational Site Number :2500010 | Nantes , France, 44093Investigational Site Number :2500002 | Nice , France, 06002Investigational Site Number :2500017 | Nîmes , France, 30029Investigational Site Number :2500007 | Paris , France, 75019Investigational Site Number :2500004 | Poissy , France, 78300Investigational Site Number :2500003 | Rennes , France, 35033Investigational Site Number :2500001 | Strasbourg , France, 67098Investigational Site Number :2760005 | Bayreuth , Germany, 95445Investigational Site Number :2760015 | Berlin , Germany, 10713Investigational Site Number :2760014 | Berlin , Germany, 12099Investigational Site Number :2760020 | Bochum , Germany, 44791Investigational Site Number :2760012 | Essen , Germany, 45147Investigational Site Number :2760003 | Würzburg , Germany, 97070Investigational Site Number :3000001 | Athens , Greece, 115 28Investigational Site Number :3000006 | Athens , Greece, 11535Investigational Site Number :3000002 | Athens , Greece, 12462Investigational Site Number :3000007 | Athens , Greece, 15125Investigational Site Number :3000009 | Athens , Greece, Investigational Site Number :3000004 | Larissa , Greece, 41110Investigational Site Number :3000003 | Thessaloniki , Greece, 546 36Investigational Site Number :3480105 | Budapest , Hungary, 1135Investigational Site Number :3480102 | Budapest , Hungary, 1145Investigational Site Number :3480106 | Kaposvár , Hungary, 7400Investigational Site Number :3480103 | Tatabánya , Hungary, 2800Investigational Site Number :3560005 | Chandigarh , India, 160012Investigational Site Number :3560007 | Gurgaon , India, 122001Investigational Site Number :3560008 | Gurgaon , India, 122002Investigational Site Number :3560002 | New Delhi , India, 110060Investigational Site Number :3560004 | Thiruvananthapuram , India, 695004Investigational Site Number :3760002 | Ashkelon , Israel, 78278Investigational Site Number :3760003 | Haifa , Israel, 31096Investigational Site Number :3760006 | Rehovot , Israel, 76100Investigational Site Number :3760004 | Safed , Israel, 13100Investigational Site Number :3760001 | Tel Litwinsky , Israel, 52621Investigational Site Number :4280002 | Riga , Latvia, LV-1002Investigational Site Number :4280003 | Riga , Latvia, LV-1005Investigational Site Number :5280001 | Amsterdam , Netherlands, 1081 GNInvestigational Site Number :5780002 | Namsos , Norway, 7800Investigational Site Number :5780001 | Oslo , Norway, 0450Investigational Site Number :6200001 | Braga , Portugal, 4710-243Investigational Site Number :6200005 | Coimbra , Portugal, 3000-075Investigational Site Number :6200011 | Lisbon , Portugal, 1162-050Investigational Site Number :6200006 | Lisbon , Portugal, 1649-035Investigational Site Number :6200002 | Matosinhos Municipality , Portugal, 4464-513Investigational Site Number :6200010 | Porto , Portugal, 4099-001Investigational Site Number :6200004 | Santa Maria da Feira , Portugal, 4520-211San Juan MS Center-Site Number:8400015 | Guaynabo , Puerto Rico, 00969Investigational Site Number :6430006 | Barnaul , Russia, 656024Investigational Site Number :6430013 | Bryansk , Russia, 241033Investigational Site Number :6430001 | Kazan' , Russia, 420021Investigational Site Number :6430010 | Kirov , Russia, 610998Investigational Site Number :6430007 | Moscow , Russia, 117997Investigational Site Number :6430005 | Moscow , Russia, 127015Investigational Site Number :6430003 | Novosibirsk , Russia, 630087Investigational Site Number :6430014 | Saint Petersburg , Russia, 192242Investigational Site Number :6430004 | Saint Petersburg , Russia, 197022Investigational Site Number :6430002 | Saint Petersburg , Russia, 197110Investigational Site Number :6430011 | Saransk , Russia, 430032Investigational Site Number :6430012 | Yekaterinburg , Russia, 620102Investigational Site Number :6880001 | Belgrade , Serbia, 11000Investigational Site Number :6880003 | Belgrade , Serbia, 11000Investigational Site Number :6880006 | Belgrade , Serbia, 11000Investigational Site Number :6880002 | Kragujevac , Serbia, 34000Investigational Site Number :6880004 | Niš , Serbia, 18000Investigational Site Number :6880005 | Novi Sad , Serbia, 21000Investigational Site Number :7030001 | Bratislava , Slovakia, 82606Investigational Site Number :7030002 | Martin , Slovakia, 03659Investigational Site Number :7030004 | Nitra , Slovakia, 950 01Investigational Site Number :4100001 | Goyang-si Gyeonggi-do, South Korea, 10408Investigational Site Number :4100003 | Seoul Seoul-teukbyeolsi, South Korea, 03080Investigational Site Number :4100006 | Seoul Seoul-teukbyeolsi, South Korea, 03722Investigational Site Number :4100002 | Seoul Seoul-teukbyeolsi, South Korea, 06351Investigational Site Number :7240011 | Seville Andalusia, Spain, 41009Investigational Site Number :7240006 | Barcelona Barcelona [Barcelona], Spain, 08036Investigational Site Number :7240009 | Barakaldo Bizkaia, Spain, 48903Investigational Site Number :7240004 | Salt Girona [Gerona], Spain, 17190Investigational Site Number :7240013 | Las Palmas de Gran Canaria Las Palmas, Spain, 35010Investigational Site Number :7240008 | A Coruña , Spain, 15006Investigational Site Number :7240007 | L'Hospitalet de Llobregat , Spain, 08907Investigational Site Number :7240005 | Lleida , Spain, 25198Investigational Site Number :7240003 | Madrid , Spain, 28007Investigational Site Number :7240001 | Madrid , Spain, 28034Investigational Site Number :7240002 | Madrid , Spain, 28040Investigational Site Number :7240010 | Málaga , Spain, 29010Investigational Site Number :7240012 | Pozuelo de Alarcón , Spain, 28223Investigational Site Number :7560003 | Aarau , Switzerland, 5001Investigational Site Number :7560002 | Bern , Switzerland, 3010Investigational Site Number :7560004 | Lugano , Switzerland, 6903Investigational Site Number :7920002 | Ankara , Turkey (Türkiye), 06100Investigational Site Number :7920005 | Besevler / Ankara , Turkey (Türkiye), 06500Investigational Site Number :7920006 | Istanbul , Turkey (Türkiye), 34896Investigational Site Number :7920004 | Kuttahta , Turkey (Türkiye), 43100Investigational Site Number :7920001 | Samsun , Turkey (Türkiye), Investigational Site Number :7920003 | Trabzon , Turkey (Türkiye), 61080Investigational Site Number :8040020 | Chernihiv , Ukraine, 14029Investigational Site Number :8040002 | Chernivtsi , Ukraine, 58000Investigational Site Number :8040019 | Chernivtsi , Ukraine, 58023Investigational Site Number :8040005 | Dnipro , Ukraine, 49005Investigational Site Number :8040022 | Kharkiv , Ukraine, 61103Investigational Site Number :8040018 | Kharkiv , Ukraine, 61166Investigational Site Number :8040007 | Kyiv , Ukraine, 02091Investigational Site Number :8040006 | Lviv , Ukraine, 79013Investigational Site Number :8040003 | Vinnytsia , Ukraine, 21050Investigational Site Number :8260003 | Exeter Devon, United Kingdom, EX2 5DWInvestigational Site Number :8260016 | Canterbury Kent, United Kingdom, CT1 3NGInvestigational Site Number :8260009 | Bristol , United Kingdom, BS10 5NB
Investigators
Study Director: Clinical Sciences & Operations, Sanofi
Study Documents (Full Text)
Documents provided by SanofiStudy Protocol  December 19, 2023Documents provided by SanofiStatistical Analysis Plan  July 9, 2024