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Clinical Trial Details — Status: Terminated

Administrative data

NCT number NCT01047319
Other study ID # MS-LAQ-302E
Secondary ID 2009-015815-42
Status Terminated
Phase Phase 3
First received
Last updated
Start date May 27, 2010
Est. completion date June 30, 2017

Study information

Verified date December 2021
Source Teva Branded Pharmaceutical Products R&D, Inc.
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

To make laquinimod 0.6 mg available for all subjects who completed the placebo-controlled MS-LAQ-302 study according to the protocol and to evaluate the long-term safety, tolerability and effect on disease course of daily oral laquinimod 0.6 mg in subjects with relapsing multiple sclerosis.


Recruitment information / eligibility

Status Terminated
Enrollment 1047
Est. completion date June 30, 2017
Est. primary completion date June 30, 2017
Accepts healthy volunteers No
Gender All
Age group N/A and older
Eligibility Inclusion Criteria: 1. Subjects must have completed the Termination visit of MS-LAQ-302 (completion of all Termination visit activities) according to the MS-LAQ-302 protocol. 2. Women of child-bearing potential must practice an acceptable method of birth control [acceptable methods of birth control in this open label extension phase include: surgical sterilization, intrauterine devices, oral contraceptive, contraceptive patch (or hormone-releasing vaginal ring), long-acting injectable contraceptive, partner's vasectomy or double-barrier method (condom or diaphragm with spermicide)] during the study and up to 30 days after the last dose of the study drug.. 3. Subjects must be willing and able to comply with the protocol requirements for the duration of the study. 4. Subjects must be able to comprehend, sign and date a written informed consent prior to entering the MS-LAQ-302E study. Exclusion Criteria: 1. Premature discontinuation from the MS-LAQ-302 study, for any reason. 2. Pregnancy [according to urine dipstick ß-HCG test performed at Baseline (Month 0E) visit] or breastfeeding. 3. Subjects with clinically significant or unstable medical or surgical condition detected or worsened during the MS-LAQ-302 study, which preclude safe participation and completion of the MS-LAQ-302E study. Acute exacerbation of MS will not exclude participation in the MS-LAQ-302E study. 4. Use of inhibitors of CYP3A4 within 2 weeks prior to baseline visit (V0E, Month 0E).

Study Design


Intervention

Drug:
Laquinimod
One capsule containing 0.6 mg laquinimod to be administered orally once daily.

Locations

Country Name City State
Bulgaria Teva Investigational Site 5914 Pleven
Bulgaria Teva Investigational Site 5915 Pleven
Bulgaria Teva Investigational Site 5917 Plovdiv
Bulgaria Teva Investigational Site 4212 Ruse
Bulgaria Teva Investigational Site 5916 Shumen
Bulgaria Teva Investigational Site 5906 Sofia
Bulgaria Teva Investigational Site 5907 Sofia
Bulgaria Teva Investigational Site 5908 Sofia
Bulgaria Teva Investigational Site 5909 Sofia
Bulgaria Teva Investigational Site 5910 Sofia
Bulgaria Teva Investigational Site 5911 Sofia
Bulgaria Teva Investigational Site 5912 Sofia
Bulgaria Teva Investigational Site 5919 Sofia
Bulgaria Teva Investigational Site 5920 Sofia
Bulgaria Teva Investigational Site 5918 Stara Zagora
Bulgaria Teva Investigational Site 5913 Varna
Bulgaria Teva Investigational Site 4211 Veliko Tarnovo
Croatia Teva Investigational Site 6003 Osijek
Croatia Teva Investigational Site 6005 Varazdin
Croatia Teva Investigational Site 6001 Zagreb
Croatia Teva Investigational Site 6002 Zagreb
Croatia Teva Investigational Site 6006 Zagreb
Czechia Teva Investigational Site 5419 Olomouc
Czechia Teva Investigational Site 5418 Praha 2
Czechia Teva Investigational Site 5420 Praha 5- Motol
Czechia Teva Investigational Site 5421 Teplice
Estonia Teva Investigational Site 5508 Kohtla-Jarve
Estonia Teva Investigational Site 5507 Tallinn
Estonia Teva Investigational Site 5509 Tartu
Georgia Teva Investigational Site 8102 Tbilisi
Georgia Teva Investigational Site 8103 Tbilisi
Georgia Teva Investigational Site 8104 Tbilisi
Germany Teva Investigational Site 6402 Berlin
Germany Teva Investigational Site 6703 Berlin
Germany Teva Investigational Site 6400 Ulm
Israel Teva Investigational Site 8041 Jerusalem
Israel Teva Investigational Site 8040 Ramat Gan
Italy Teva Investigational Site 3056 Bologna
Italy Teva Investigational Site 3053 Cefalu
Italy Teva Investigational Site 3054 Chieti
Italy Teva Investigational Site 3061 Empoli
Italy Teva Investigational Site 3049 Firenze
Italy Teva Investigational Site 3055 Napoli
Italy Teva Investigational Site 3048 Rome
Italy Teva Investigational Site 3050 Rome
Italy Teva Investigational Site 3052 Rome
Lithuania Teva Investigational Site 5708 Kaunas
Lithuania Teva Investigational Site 5707 Siauliai
North Macedonia Teva Investigational Site 6500 Skopje
North Macedonia Teva Investigational Site 6501 Skopje
North Macedonia Teva Investigational Site 6502 Skopje
Poland Teva Investigational Site 5337 Bialystok
Poland Teva Investigational Site 5329 Gdansk
Poland Teva Investigational Site 5338 Gdansk
Poland Teva Investigational Site 6602 Gorzow Wielkopolski
Poland Teva Investigational Site 5333 Grodzisk Mazowiecki
Poland Teva Investigational Site 5334 Katowice
Poland Teva Investigational Site 5339 Katowice
Poland Teva Investigational Site 6603 Kielce
Poland Teva Investigational Site 4213 Konskie
Poland Teva Investigational Site 5332 Koscierzyna
Poland Teva Investigational Site 5345 Krakow
Poland Teva Investigational Site 5328 Lodz
Poland Teva Investigational Site 5330 Olsztyn
Poland Teva Investigational Site 5331 Szczecin
Poland Teva Investigational Site 5336 Warsaw
Poland Teva Investigational Site 5340 Warszawa
Poland Teva Investigational Site 5341 Warszawa
Poland Teva Investigational Site 5335 Wroclaw
Romania Teva Investigational Site 5235 Balotesti
Romania Teva Investigational Site 5218 Bucharest
Romania Teva Investigational Site 5213 Bucuresti
Romania Teva Investigational Site 5214 Bucuresti
Romania Teva Investigational Site 5215 Cluj-Napoca
Romania Teva Investigational Site 5217 Constanta
Romania Teva Investigational Site 8209 Craiova
Romania Teva Investigational Site 5216 Iasi
Romania Teva Investigational Site 5219 Sibiu
Russian Federation Teva Investigational Site 5043 Barnaul
Russian Federation Teva Investigational Site 5032 Moscow
Russian Federation Teva Investigational Site 5033 Moscow
Russian Federation Teva Investigational Site 5041 Moscow
Russian Federation Teva Investigational Site 5038 Novosibirsk
Russian Federation Teva Investigational Site 5042 Novosibirsk
Russian Federation Teva Investigational Site 5035 Saint Petersburg
Russian Federation Teva Investigational Site 5037 Samara
Russian Federation Teva Investigational Site 5034 St. Petersburg
Russian Federation Teva Investigational Site 5036 St. Petersburg
Russian Federation Teva Investigational Site 5044 Ufa
Slovakia Teva Investigational Site 6200 Bratislava
Slovakia Teva Investigational Site 6201 Bratislava
Slovakia Teva Investigational Site 6202 Nitra
Slovakia Teva Investigational Site 6203 Zilina
South Africa Teva Investigational Site 9007 Bloemfontein
South Africa Teva Investigational Site 9001 Cape Town
South Africa Teva Investigational Site 9004 Johannesburg
South Africa Teva Investigational Site 9003 Parktown- Johannesburg
South Africa Teva Investigational Site 9008 Pietermaritzburg
South Africa Teva Investigational Site 9005 Pretoria
South Africa Teva Investigational Site 9006 Rosebank
Spain Teva Investigational Site 3147 Barcelona
Spain Teva Investigational Site 3154 Figueres-Girona
Spain Teva Investigational Site 3149 L'Hospitalet de Llobregat
Spain Teva Investigational Site 3152 Madrid
Spain Teva Investigational Site 3151 Malaga
Spain Teva Investigational Site 3148 Sevilla
Spain Teva Investigational Site 3153 Tortosa-Tarragona
Ukraine Teva Investigational Site 6503 Chernihiv
Ukraine Teva Investigational Site 5823 Chernivtsi
Ukraine Teva Investigational Site 5811 Dnipropetrovsk
Ukraine Teva Investigational Site 5812 Donetsk
Ukraine Teva Investigational Site 5814 Ivano-Frankivsk
Ukraine Teva Investigational Site 5815 Kharkiv
Ukraine Teva Investigational Site 5817 Kharkiv
Ukraine Teva Investigational Site 5818 Kharkiv
Ukraine Teva Investigational Site 5822 Kyiv
Ukraine Teva Investigational Site 5809 Lviv
Ukraine Teva Investigational Site 5820 Odessa
Ukraine Teva Investigational Site 5821 Poltava
Ukraine Teva Investigational Site 5810 Vinnytsya
Ukraine Teva Investigational Site 5816 Zaporizhzhya
Ukraine Teva Investigational Site 5819 Zaporizhzhya
United States Teva Investigational Site 1261 Akron Ohio
United States Teva Investigational Site 1273 Albany New York
United States Teva Investigational Site 1264 Amherst New York
United States Teva Investigational Site 1275 Atlanta Georgia
United States Teva Investigational Site 1280 Aurora Colorado
United States Teva Investigational Site 1269 Baltimore Maryland
United States Teva Investigational Site 1245 Cleveland Ohio
United States Teva Investigational Site 1247 Columbus Ohio
United States Teva Investigational Site 1267 Homewood Alabama
United States Teva Investigational Site 1260 Indianapolis Indiana
United States Teva Investigational Site 1281 Nashville Tennessee
United States Teva Investigational Site 1272 Pasadena California
United States Teva Investigational Site 1250 Peoria Illinois
United States Teva Investigational Site 1237 Phoenix Arizona
United States Teva Investigational Site 1279 Phoenix Arizona
United States Teva Investigational Site 1244 Portland Oregon
United States Teva Investigational Site 1270 Roanoke Virginia
United States Teva Investigational Site 1238 Sacramento California
United States Teva Investigational Site 1282 Sarasota Florida
United States Teva Investigational Site 1263 Shreveport Louisiana
United States Teva Investigational Site 1253 Tacoma Washington
United States Teva Investigational Site 1276 Tucson Arizona

Sponsors (1)

Lead Sponsor Collaborator
Teva Branded Pharmaceutical Products R&D, Inc.

Countries where clinical trial is conducted

United States,  Bulgaria,  Croatia,  Czechia,  Estonia,  Georgia,  Germany,  Israel,  Italy,  Lithuania,  North Macedonia,  Poland,  Romania,  Russian Federation,  Slovakia,  South Africa,  Spain,  Ukraine, 

Outcome

Type Measure Description Time frame Safety issue
Primary Participants With Treatment-Emergent Adverse Events (TEAEs) A treatment-emergent adverse event was defined as any untoward medical occurrence that develops or worsens in severity following start of treatment 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 normal daily activities. Relation of AE to treatment was determined by the investigator. Serious AEs (SAE) 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. TEAEs associated with cancer, ischemic heart disease, cerebrovascular events, and arthritis were considered to be of special interest. Day 1 up to 7.13 years
Secondary Participants With Potentially Clinically Significant Abnormal Vital Signs Vital signs with potentially clinically significant abnormal results were evaluated using the following significance criteria:
Pulse rate: >=120 and increase >=30 beats/minute
Systolic blood pressure low: <=90 and decrease >=30 mmHg
Systolic blood pressure high: >=180 and increase >=30 mmHg
Diastolic blood pressure low: <=50 and decrease >=20 mmHg
Diastolic blood pressure high: >=100 and increase >=20 mmHg
Note that the change is compared to baseline,
Baseline (Day 0 for extension), Day 1 up to 7.13 years
Secondary Participants With Serum Chemistry Laboratory Tests That Were Potentially Clinically Significant (PCS) Abnormal Comparing Baseline to Any Time During the Study Counts include two conditions:
a change from High / Non-PCS at baseline to Low PCS at any point during the study
a change from Low / Non-PCS at baseline to High PCS at any point during the study
Participants whose condition was not changed from baseline or was changed to a non-PCS value are included in the population count.
ALT=alanine aminotransferase ALP=alkaline phosphatase P-amylase=amylase, pancreatic AST=aspartate aminotransferase CRP=C reactive protein CK=creatine kinase CTN=creatinine FIB=fibrinogen GGT=gamma glutamyl transferase K=potassium
Baseline (Day 0), Day 1 to 7.13 years
Secondary Participants With Serum Hematology Laboratory Tests That Were Potentially Clinically Significant (PCS) Abnormal Comparing Baseline to Any Time During the Study Counts include two conditions:
a change from High / Non-PCS at baseline to Low PCS at any point during the study
a change from Low / Non-PCS at baseline to High PCS at any point during the study
Participants whose condition was not changed from baseline or was changed to a non-PCS value are included in the population count.
Baseline (Day 0), Day 1 to 7.13 years
Secondary Participants With Electrocardiogram (ECG) Fiindings That Shifted From Baseline to Any Time During the Study Shifts are presented as Baseline finding / Worse finding at anytime during the study.
Categories for findings are:
normal
abnormal, not clinically significant (Not CS)
abnormal, clinically significant (CS)
Baseline (Day 0), Day 1 to 7.13 years
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