- ICH GCP
- US Clinical Trials Registry
- Clinical Trial NCT02629861
Efficacy and Safety of 2 Dose Regimens of TEV-48125 Versus Placebo for the Preventive Treatment of Episodic Migraine
A Multicenter, Randomized, Double-Blind, Placebo-Controlled, Parallel-Group Study Comparing the Efficacy and Safety of 2 Dose Regimens of Subcutaneous Administration of Fremanezumab (TEV-48125) vs Placebo for the Preventive Treatment of Episodic Migraine
Study Overview
Study Type
Enrollment (Actual)
Phase
- Phase 3
Contacts and Locations
Study Locations
-
-
-
Calgary, Canada, T3M 1M4
- Teva Investigational Site 11120
-
Calgary, Canada
- Teva Investigational Site 11120
-
Montreal, Canada, H2W 1V1
- Teva Investigational Site 11121
-
Montreal, Canada
- Teva Investigational Site 11121
-
Newmarket, Canada, L3Y5G8
- Teva Investigational Site 11122
-
Newmarket, Canada
- Teva Investigational Site 11122
-
Sarnia, Canada, N7T 4X3
- Teva Investigational Site 11123
-
Sarnia, Canada
- Teva Investigational Site 11123
-
-
Ontario
-
Hamilton, Ontario, Canada, L8N 1Y2
- Teva Investigational Site 11124
-
Hamilton, Ontario, Canada
- Teva Investigational Site 11124
-
-
-
-
-
Brno, Czechia, 602 00
- Teva Investigational Site 54144
-
Brno, Czechia
- Teva Investigational Site 54144
-
Kunratice, Czechia, 14800
- Teva Investigational Site 54141
-
Kunratice, Czechia
- Teva Investigational Site 54141
-
Pardubice, Czechia, 53002
- Teva Investigational Site 54145
-
Pardubice, Czechia
- Teva Investigational Site 54145
-
Prague 4, Czechia, 140 59
- Teva Investigational Site 54142
-
Prague-4-Krc, Czechia
- Teva Investigational Site 54142
-
Praha, Czechia, 100 00
- Teva Investigational Site 54143
-
Praha, Czechia
- Teva Investigational Site 54143
-
Praha 3, Czechia, 130 00
- Teva Investigational Site 54146
-
Praha 3, Czechia
- Teva Investigational Site 54146
-
-
-
-
-
Helsinki, Finland, 00100
- Teva Investigational Site 40018
-
Helsinki, Finland, 00930
- Teva Investigational Site 40017
-
Helsinki, Finland
- Teva Investigational Site 40017
-
Helsinki, Finland
- Teva Investigational Site 40018
-
Turku, Finland, 20100
- Teva Investigational Site 40016
-
Turku, Finland
- Teva Investigational Site 40016
-
-
-
-
-
Holon, Israel, 58100
- Teva Investigational Site 80096
-
Holon, Israel
- Teva Investigational Site 80096
-
Jerusalem, Israel, 9112001
- Teva Investigational Site 80099
-
Jerusalem, Israel
- Teva Investigational Site 80099
-
Nahariya, Israel, 221001
- Teva Investigational Site 80098
-
Nahariya, Israel
- Teva Investigational Site 80098
-
Netanya, Israel, 4244916
- Teva Investigational Site 80097
-
Netanya, Israel
- Teva Investigational Site 80097
-
Ramat Gan, Israel, 5262160
- Teva Investigational Site 80100
-
Ramat Gan, Israel
- Teva Investigational Site 80100
-
Tel Aviv, Israel, 64239
- Teva Investigational Site 80095
-
Tel Aviv, Israel
- Teva Investigational Site 80095
-
-
-
-
-
Chofu-shi, Japan, 182-0006
- Teva Investigational Site 84072
-
Chofu-shi, Japan
- Teva Investigational Site 84064
-
Chofu-shi, Japan
- Teva Investigational Site 84072
-
Kagoshima, Japan, 892-0844
- Teva Investigational Site 84066
-
Kagoshima-shi, Japan
- Teva Investigational Site 84066
-
Kai, Japan, 400-0124
- Teva Investigational Site 84069
-
Kai-shi, Japan
- Teva Investigational Site 84069
-
Kawasaki, Japan, 211-8588
- Teva Investigational Site 84073
-
Kawasaki-shi, Japan
- Teva Investigational Site 84073
-
Kyoto, Japan, 600-8811
- Teva Investigational Site 84067
-
Kyoto, Japan
- Teva Investigational Site 84067
-
Osaka-shi, Japan, 556-0015
- Teva Investigational Site 84062
-
Osaka-shi, Japan
- Teva Investigational Site 84062
-
Saitama, Japan, 338-8577
- Teva Investigational Site 84070
-
Saitama-shi, Japan
- Teva Investigational Site 84070
-
Sendai-shi, Japan, 982-0014
- Teva Investigational Site 84061
-
Sendai-shi, Japan
- Teva Investigational Site 84061
-
Shimotsuma, Japan
- Teva Investigational Site 84065
-
Shinjuku-ku, Japan, 160-8582
- Teva Investigational Site 84063
-
Shizuoka, Japan, 4200-853
- Teva Investigational Site 84068
-
Shizuoka-shi, Japan
- Teva Investigational Site 84068
-
Tochigi, Japan, 321-0293
- Teva Investigational Site 84065
-
Tokyo, Japan, 182-0006
- Teva Investigational Site 84064
-
Toyonaka, Japan
- Teva Investigational Site 84071
-
Toyonaka-shi, Japan
- Teva Investigational Site 84071
-
-
-
-
-
Krakow, Poland, 31-523
- Teva Investigational Site 53364
-
Krakow, Poland, 33-332
- Teva Investigational Site 53363
-
Krakow, Poland
- Teva Investigational Site 53363
-
Krakow, Poland
- Teva Investigational Site 53364
-
Lublin, Poland, 20-022
- Teva Investigational Site 53366
-
Lublin, Poland
- Teva Investigational Site 53366
-
Poznan, Poland, 60-529
- Teva Investigational Site 53365
-
Poznan, Poland
- Teva Investigational Site 53365
-
Warsaw, Poland, 04-730
- Teva Investigational Site 53367
-
Warsaw, Poland
- Teva Investigational Site 53367
-
-
-
-
-
Kazan, Russian Federation, 420012
- Teva Investigational Site 50399
-
Kazan, Russian Federation, 420021
- Teva Investigational Site 50395
-
Kazan, Russian Federation
- Teva Investigational Site 50395
-
Kazan, Russian Federation
- Teva Investigational Site 50399
-
Moscow, Russian Federation, 121467
- Teva Investigational Site 50394
-
Moscow, Russian Federation, 129128
- Teva Investigational Site 50400
-
Moscow, Russian Federation
- Teva Investigational Site 50394
-
Moscow, Russian Federation
- Teva Investigational Site 50400
-
Nizhniy Novgorod, Russian Federation, 603126
- Teva Investigational Site 50398
-
Nizhniy Novgorod, Russian Federation, 603137
- Teva Investigational Site 50396
-
Nizhniy Novgorod, Russian Federation
- Teva Investigational Site 50396
-
Nizhniy Novgorod, Russian Federation
- Teva Investigational Site 50398
-
Ufa, Russian Federation, 450007
- Teva Investigational Site 50397
-
Ufa, Russian Federation
- Teva Investigational Site 50397
-
-
-
-
-
Madrid, Spain, 28046
- Teva Investigational Site 31207
-
Madrid, Spain
- Teva Investigational Site 31207
-
Pamplona, Spain, 31008
- Teva Investigational Site 31208
-
Pamplona, Spain
- Teva Investigational Site 31208
-
Valladolid, Spain, 47003
- Teva Investigational Site 31205
-
Valladolid, Spain
- Teva Investigational Site 31205
-
Zaragoza, Spain, 50009
- Teva Investigational Site 31206
-
Zaragoza, Spain
- Teva Investigational Site 31206
-
-
-
-
Alabama
-
Birmingham, Alabama, United States, 35211
- Teva Investigational Site 13628
-
Birmingham, Alabama, United States, 35216
- Teva Investigational Site 13577
-
Birmingham, Alabama, United States
- Teva Investigational Site 13577
-
Birmingham, Alabama, United States
- Teva Investigational Site 13628
-
-
Arizona
-
Phoenix, Arizona, United States, 85018
- Teva Investigational Site 13606
-
Phoenix, Arizona, United States, 85023
- Teva Investigational Site 13579
-
Phoenix, Arizona, United States
- Teva Investigational Site 13579
-
Phoenix, Arizona, United States
- Teva Investigational Site 13606
-
-
Arkansas
-
Little Rock, Arkansas, United States, 72205
- Teva Investigational Site 13602
-
Little Rock, Arkansas, United States
- Teva Investigational Site 13602
-
-
California
-
Encino, California, United States, 91316
- Teva Investigational Site 13568
-
Encino, California, United States
- Teva Investigational Site 13568
-
Fullerton, California, United States, 92835
- Teva Investigational Site 13546
-
Fullerton, California, United States
- Teva Investigational Site 13546
-
Long Beach, California, United States, 90806
- Teva Investigational Site 13540
-
Long Beach, California, United States
- Teva Investigational Site 13540
-
Redlands, California, United States, 92374
- Teva Investigational Site 13632
-
Redlands, California, United States
- Teva Investigational Site 13632
-
Redondo Beach, California, United States, 90277
- Teva Investigational Site 13571
-
Redondo Beach, California, United States
- Teva Investigational Site 13571
-
San Diego, California, United States, 92103
- Teva Investigational Site 13573
-
San Diego, California, United States
- Teva Investigational Site 13573
-
Santa Monica, California, United States, 90404
- Teva Investigational Site 13538
-
Santa Monica, California, United States
- Teva Investigational Site 13538
-
Santa Rosa, California, United States, 95405
- Teva Investigational Site 13594
-
Santa Rosa, California, United States
- Teva Investigational Site 13594
-
Walnut Creek, California, United States, 94598
- Teva Investigational Site 13595
-
Walnut Creek, California, United States
- Teva Investigational Site 13595
-
-
Colorado
-
Aurora, Colorado, United States, 80014
- Teva Investigational Site 13629
-
Aurora, Colorado, United States
- Teva Investigational Site 13629
-
Boulder, Colorado, United States, 80301
- Teva Investigational Site 13557
-
Boulder, Colorado, United States
- Teva Investigational Site 13557
-
Colorado Springs, Colorado, United States, 80918
- Teva Investigational Site 13593
-
Colorado Springs, Colorado, United States
- Teva Investigational Site 13593
-
Denver, Colorado, United States, 80210
- Teva Investigational Site 13633
-
Denver, Colorado, United States, 80239
- Teva Investigational Site 13612
-
Denver, Colorado, United States
- Teva Investigational Site 13612
-
Denver, Colorado, United States
- Teva Investigational Site 13633
-
Englewood, Colorado, United States, 80113
- Teva Investigational Site 13631
-
Englewood, Colorado, United States
- Teva Investigational Site 13631
-
-
Connecticut
-
East Hartford, Connecticut, United States, 06118
- Teva Investigational Site 13563
-
East Hartford, Connecticut, United States
- Teva Investigational Site 13563
-
Stamford, Connecticut, United States, 06905
- Teva Investigational Site 13550
-
Stamford, Connecticut, United States
- Teva Investigational Site 13550
-
-
Florida
-
Bradenton, Florida, United States, 34201
- Teva Investigational Site 13635
-
Bradenton, Florida, United States
- Teva Investigational Site 13635
-
Gainesville, Florida, United States, 32607
- Teva Investigational Site 13597
-
Gainesville, Florida, United States
- Teva Investigational Site 13597
-
Hialeah, Florida, United States, 33012
- Teva Investigational Site 13607
-
Hialeah, Florida, United States
- Teva Investigational Site 13607
-
Jacksonville, Florida, United States, 32205
- Teva Investigational Site 13559
-
Jacksonville, Florida, United States
- Teva Investigational Site 13559
-
Ocala, Florida, United States, 34471
- Teva Investigational Site 13584
-
Ocala, Florida, United States
- Teva Investigational Site 13584
-
Orlando, Florida, United States, 32806
- Teva Investigational Site 13587
-
Orlando, Florida, United States
- Teva Investigational Site 13551
-
Orlando, Florida, United States
- Teva Investigational Site 13555
-
Orlando, Florida, United States
- Teva Investigational Site 13587
-
Orlando, Florida, United States
- Teva Investigational Site 13599
-
Pembroke Pines, Florida, United States, 33026
- Teva Investigational Site 13553
-
Pembroke Pines, Florida, United States
- Teva Investigational Site 13553
-
Pinellas Park, Florida, United States, 33781
- Teva Investigational Site 13616
-
Pinellas Park, Florida, United States
- Teva Investigational Site 13616
-
West Palm Beach, Florida, United States, 33407
- Teva Investigational Site 13567
-
West Palm Beach, Florida, United States
- Teva Investigational Site 13567
-
-
Georgia
-
Atlanta, Georgia, United States, 30312
- Teva Investigational Site 13620
-
Atlanta, Georgia, United States, 30342
- Teva Investigational Site 13537
-
Atlanta, Georgia, United States
- Teva Investigational Site 13537
-
Atlanta, Georgia, United States
- Teva Investigational Site 13620
-
-
Idaho
-
Boise, Idaho, United States, 83642
- Teva Investigational Site 13604
-
Meridian, Idaho, United States
- Teva Investigational Site 13604
-
-
Illinois
-
Chicago, Illinois, United States, 60607
- Teva Investigational Site 13585
-
Chicago, Illinois, United States, 60654
- Teva Investigational Site 13621
-
Chicago, Illinois, United States
- Teva Investigational Site 13585
-
Chicago, Illinois, United States
- Teva Investigational Site 13621
-
Evanston, Illinois, United States, 60201
- Teva Investigational Site 13627
-
Evanston, Illinois, United States
- Teva Investigational Site 13627
-
-
Indiana
-
Indianapolis, Indiana, United States, 46254
- Teva Investigational Site 13596
-
Indianapolis, Indiana, United States
- Teva Investigational Site 13596
-
-
Kansas
-
Wichita, Kansas, United States, 67207
- Teva Investigational Site 13617
-
Wichita, Kansas, United States, 67211
- Teva Investigational Site 13598
-
Wichita, Kansas, United States
- Teva Investigational Site 13598
-
Wichita, Kansas, United States
- Teva Investigational Site 13617
-
-
Kentucky
-
Louisville, Kentucky, United States, 40207
- Teva Investigational Site 13566
-
Louisville, Kentucky, United States
- Teva Investigational Site 13566
-
-
Louisiana
-
Metairie, Louisiana, United States, 70006
- Teva Investigational Site 13603
-
Metairie, Louisiana, United States
- Teva Investigational Site 13603
-
-
Maryland
-
Baltimore, Maryland, United States
- Teva Investigational Site 13582
-
Pikesville, Maryland, United States, 21208
- Teva Investigational Site 13582
-
-
Massachusetts
-
Boston, Massachusetts, United States, 02131
- Teva Investigational Site 13590
-
Boston, Massachusetts, United States
- Teva Investigational Site 13590
-
New Bedford, Massachusetts, United States, 02301
- Teva Investigational Site 13589
-
New Bedford, Massachusetts, United States
- Teva Investigational Site 13589
-
Wellesley Hills, Massachusetts, United States, 02481
- Teva Investigational Site 13543
-
Wellesley Hills, Massachusetts, United States
- Teva Investigational Site 13543
-
-
Michigan
-
Ann Arbor, Michigan, United States, 48104
- Teva Investigational Site 13539
-
Ann Arbor, Michigan, United States
- Teva Investigational Site 13539
-
-
Minnesota
-
Golden Valley, Minnesota, United States, 55422
- Teva Investigational Site 13542
-
Golden Valley, Minnesota, United States
- Teva Investigational Site 13542
-
-
Missouri
-
Kansas City, Missouri, United States, 64114
- Teva Investigational Site 13534
-
Kansas City, Missouri, United States
- Teva Investigational Site 13534
-
Saint Louis, Missouri, United States, 63141
- Teva Investigational Site 13619
-
Saint Louis, Missouri, United States
- Teva Investigational Site 13619
-
Springfield, Missouri, United States
- Teva Investigational Site 13536
-
-
Nebraska
-
Fremont, Nebraska, United States, 68025
- Teva Investigational Site 13618
-
Fremont, Nebraska, United States
- Teva Investigational Site 13618
-
-
Nevada
-
Las Vegas, Nevada, United States, 89106
- Teva Investigational Site 13605
-
Las Vegas, Nevada, United States
- Teva Investigational Site 13605
-
-
New Hampshire
-
Lebanon, New Hampshire, United States, 03756
- Teva Investigational Site 13578
-
Lebanon, New Hampshire, United States
- Teva Investigational Site 13578
-
-
New Jersey
-
Martinsville, New Jersey, United States
- Teva Investigational Site 13575
-
Raritan, New Jersey, United States, 08869
- Teva Investigational Site 13575
-
-
New Mexico
-
Albuquerque, New Mexico, United States, 87102
- Teva Investigational Site 13588
-
Albuquerque, New Mexico, United States
- Teva Investigational Site 13588
-
-
New York
-
Amherst, New York, United States, 14226
- Teva Investigational Site 13576
-
Amherst, New York, United States
- Teva Investigational Site 13576
-
Plainview, New York, United States, 11803
- Teva Investigational Site 13565
-
Plainview, New York, United States
- Teva Investigational Site 13565
-
-
North Carolina
-
Greensboro, North Carolina, United States, 27401
- Teva Investigational Site 13544
-
Greensboro, North Carolina, United States, 27408
- Teva Investigational Site 13574
-
Greensboro, North Carolina, United States
- Teva Investigational Site 13544
-
Greensboro, North Carolina, United States
- Teva Investigational Site 13574
-
Raleigh, North Carolina, United States, 27607
- Teva Investigational Site 13545
-
Raleigh, North Carolina, United States
- Teva Investigational Site 13545
-
-
Ohio
-
Akron, Ohio, United States, 44311
- Teva Investigational Site 13609
-
Akron, Ohio, United States, 44311
- Teva Investigational Site 13634
-
Akron, Ohio, United States
- Teva Investigational Site 13609
-
Akron, Ohio, United States
- Teva Investigational Site 13634
-
Cincinnati, Ohio, United States, 45227
- Teva Investigational Site 13533
-
Cincinnati, Ohio, United States, 45249
- Teva Investigational Site 13624
-
Cincinnati, Ohio, United States
- Teva Investigational Site 13533
-
Cincinnati, Ohio, United States
- Teva Investigational Site 13624
-
Cleveland, Ohio, United States, 44195
- Teva Investigational Site 13569
-
Cleveland, Ohio, United States
- Teva Investigational Site 13569
-
Columbus, Ohio, United States, 43212
- Teva Investigational Site 13626
-
Columbus, Ohio, United States
- Teva Investigational Site 13626
-
Mogadore, Ohio, United States, 44260
- Teva Investigational Site 13625
-
Mogadore, Ohio, United States
- Teva Investigational Site 13625
-
-
Oklahoma
-
Oklahoma City, Oklahoma, United States, 73112
- Teva Investigational Site 13561
-
Oklahoma City, Oklahoma, United States
- Teva Investigational Site 13561
-
-
Oregon
-
Eugene, Oregon, United States, 97401
- Teva Investigational Site 13601
-
Eugene, Oregon, United States
- Teva Investigational Site 13601
-
-
Pennsylvania
-
Jenkintown, Pennsylvania, United States, 19046
- Teva Investigational Site 13591
-
Jenkintown, Pennsylvania, United States
- Teva Investigational Site 13591
-
Philadelphia, Pennsylvania, United States, 19107
- Teva Investigational Site 13554
-
Philadelphia, Pennsylvania, United States
- Teva Investigational Site 13554
-
Uniontown, Pennsylvania, United States, 15401
- Teva Investigational Site 13608
-
Uniontown, Pennsylvania, United States
- Teva Investigational Site 13608
-
-
South Carolina
-
Greer, South Carolina, United States, 29650
- Teva Investigational Site 13615
-
Greer, South Carolina, United States
- Teva Investigational Site 13615
-
Mount Pleasant, South Carolina, United States, 29464
- Teva Investigational Site 13556
-
Mount Pleasant, South Carolina, United States
- Teva Investigational Site 13556
-
-
Tennessee
-
Bristol, Tennessee, United States, 37620
- Teva Investigational Site 13560
-
Bristol, Tennessee, United States
- Teva Investigational Site 13560
-
Nashville, Tennessee, United States, 37203
- Teva Investigational Site 13532
-
Nashville, Tennessee, United States, 37203
- Teva Investigational Site 13552
-
Nashville, Tennessee, United States
- Teva Investigational Site 13532
-
Nashville, Tennessee, United States
- Teva Investigational Site 13552
-
-
Texas
-
Austin, Texas, United States, 78731
- Teva Investigational Site 13541
-
Austin, Texas, United States
- Teva Investigational Site 13541
-
Dallas, Texas, United States, 75214
- Teva Investigational Site 13623
-
Dallas, Texas, United States
- Teva Investigational Site 13623
-
Plano, Texas, United States, 75024
- Teva Investigational Site 13611
-
Plano, Texas, United States
- Teva Investigational Site 13611
-
San Antonio, Texas, United States, 78229
- Teva Investigational Site 13572
-
San Antonio, Texas, United States
- Teva Investigational Site 13572
-
-
Utah
-
Murray, Utah, United States, 84107
- Teva Investigational Site 13614
-
Murray, Utah, United States
- Teva Investigational Site 13614
-
West Jordan, Utah, United States, 84088
- Teva Investigational Site 13581
-
West Jordan, Utah, United States
- Teva Investigational Site 13581
-
-
Virginia
-
Virginia Beach, Virginia, United States, 23454
- Teva Investigational Site 13630
-
Virginia Beach, Virginia, United States
- Teva Investigational Site 13630
-
-
Washington
-
Seattle, Washington, United States, 98105
- Teva Investigational Site 13564
-
Seattle, Washington, United States, 98105
- Teva Investigational Site 13586
-
Seattle, Washington, United States
- Teva Investigational Site 13564
-
Seattle, Washington, United States
- Teva Investigational Site 13586
-
-
West Virginia
-
Morgantown, West Virginia, United States, 26506
- Teva Investigational Site 13600
-
Morgantown, West Virginia, United States
- Teva Investigational Site 13600
-
-
Participation Criteria
Eligibility Criteria
Ages Eligible for Study
Accepts Healthy Volunteers
Genders Eligible for Study
Description
Inclusion Criteria:
- Males or females aged 18 to 70 years, inclusive, with migraine onset at ≤50 years of age
- Patient signs and dates the informed consent document
- Patient has history of migraine according to International Classification of Headache Disorders, or clinical judgment suggests a migraine diagnosis
- 85% e-diary compliance
Total body weight between 99 and 265 lbs, inclusive
- Additional criteria apply, please contact the investigator for more information
Exclusion Criteria:
- Clinically significant hematological, cardiac, renal, endocrine, pulmonary, gastrointestinal, genitourinary, neurologic, hepatic, or ocular disease, at the discretion of the investigator
- Evidence or medical history of clinically significant psychiatric issues, including any suicide attempt in the past, or suicidal ideation with a specific plan in the past 2 years
- History of clinically significant cardiovascular disease or vascular ischemia (such as myocardial, neurological [eg, cerebral ischemia], peripheral extremity ischemia, or other ischemic event) or thromboembolic events (arterial or venous thrombotic or embolic events), such as cerebrovascular accident (including transient ischemic attacks), deep vein thrombosis, or pulmonary embolism
- Known infection or history of human immunodeficiency virus, tuberculosis, or chronic hepatitis B or C infection
- Past or current history of cancer in the last 5 years, except for appropriately treated nonmelanoma skin carcinoma
- Pregnant or nursing females
- History of hypersensitivity reactions to injected proteins, including monoclonal antibodies
Participation in a clinical study of a new chemical entity or a prescription medicine within 2 months or 5 half-lives, whichever is longer
- Additional criteria apply, please contact the investigator for more information
Study Plan
How is the study designed?
Design Details
- Primary Purpose: Treatment
- Allocation: Randomized
- Interventional Model: Parallel Assignment
- Masking: Quadruple
Arms and Interventions
Participant Group / Arm |
Intervention / Treatment |
---|---|
Placebo Comparator: Placebo
Matching Placebo
|
Placebo 1.5 mL pre-filled syringes identical in appearance to active intervention.
Study drug was administered at the clinical site.
|
Experimental: Fremanezumab 675 mg/placebo/placebo
Participants randomized to receive fremanezumab 675 mg/placebo/placebo received 675 mg of fremanezumab as 3 injections (225 mg/1.5 mL) on Day 0, and placebo as a single 1.5-mL injection on Days 28 and 56.
|
Placebo 1.5 mL pre-filled syringes identical in appearance to active intervention.
Study drug was administered at the clinical site.
Fremanezumab was provided as a sterile, unpreserved, aqueous solution for injection, 225 mg/1.5 mL pre-filled syringe for single-use administration. The 675 mg dose was given as 3 injections; doses of 225 mg were given as a single injection. Study drug was administered at the clinical site.
Other Names:
|
Experimental: Fremanezumab 225/225/225 mg
Participants randomized to receive fremanezumab 225/225/225 mg received 1 active injection (225 mg/1.5 mL) on Days 0, 28 and 56.
|
Fremanezumab was provided as a sterile, unpreserved, aqueous solution for injection, 225 mg/1.5 mL pre-filled syringe for single-use administration. The 675 mg dose was given as 3 injections; doses of 225 mg were given as a single injection. Study drug was administered at the clinical site.
Other Names:
|
What is the study measuring?
Primary Outcome Measures
Outcome Measure |
Measure Description |
Time Frame |
---|---|---|
Change From Baseline in the Monthly Average Number of Migraine Days During the 12-Week Period After the First Dose of Study Drug
Time Frame: Baseline (Days -28 to Day -1), Treatment (Days 1 - Week 12)
|
A migraine day was defined as when at least 1 of the following situations occurred: - a calendar day (0:00 to 23:59) demonstrating at least 4 consecutive hours of a headache endorsing criteria for migraine with or without aura - a calendar day (0:00 to 23:59) demonstrating at least 4 consecutive hours of a headache endorsing criteria for probable migraine, a migraine subtype where only 1 migraine criterion is missing - a calendar day (0:00 to 23:59) demonstrating a headache of any duration that was treated with migraine-specific medications (triptans and ergot compounds) Monthly averages are derived and normalized to 28 days equivalent by the following formula: (# days of efficacy variable over relevant period / # days with assessments recorded in the e-diary over the relevant period) * 28.
The change is calculated as postbaseline value - baseline value.
|
Baseline (Days -28 to Day -1), Treatment (Days 1 - Week 12)
|
Participants With Adverse Events
Time Frame: Day 1 to Week 12
|
An adverse event 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.
|
Day 1 to Week 12
|
Secondary Outcome Measures
Outcome Measure |
Measure Description |
Time Frame |
---|---|---|
Prothrombin Time Shifts From Baseline to Endpoint
Time Frame: Baseline (Day 0), Treatment Endpoint (Week 12)
|
Shifts in prothrombin time from baseline to endpoint were summarized using patient counts grouped into three categories: - Low (below normal range) - Normal (within the normal range of 9.4 to 12.5 seconds) - High (above normal range) Shift format is: baseline finding / endpoint finding
|
Baseline (Day 0), Treatment Endpoint (Week 12)
|
Injection Site Reaction Adverse Events
Time Frame: Day 1 to Week 12
|
Counts of participants who reported treatment-emergent injection site reactions as AEs are summarized.
Preferred terms from MedDRA version 18.1 are offered without a threshold applied.
|
Day 1 to Week 12
|
Percentage of Participants With At Least 50% Reduction In Monthly Average Number of Migraine Days During the 12-Week Period After the First Dose of Study Drug
Time Frame: Baseline (Days -28 to Day -1), Treatment Month 1, Month 2, Month 3, Month 1-3 (Days 1 - Week 12)
|
Responder rates were defined as the percentage of total subjects who reached at least a 50% reduction in the monthly average of headache days (as subjectively reported by participants in the study diary) of at least moderate severity relative to the baseline period.
For the overall analysis (Month 1-3), patients who discontinued early were considered nonresponders.
Monthly averages are derived and normalized to 28 days equivalent by the following formula: (# days of efficacy variable over relevant period / # days with assessments recorded in the e-diary over the relevant period) * 28.
The percentage reduction in monthly average is calculated as: ((baseline value - postbaseline value) / baseline value) * 100
|
Baseline (Days -28 to Day -1), Treatment Month 1, Month 2, Month 3, Month 1-3 (Days 1 - Week 12)
|
Change From Baseline in the Monthly Average Number of Days of Use of Any Acute Headache Medicine During the 12 Week Period After the First Dose of Study Drug
Time Frame: Baseline (Days -28 to Day -1), Treatment (Days 1 - Week 12)
|
Patients recorded any migraine medications (name of drug, number of tablets/capsules, and the dose in milligrams per tablet/capsule) taken on each day in their electronic headache diary device.
Acute migraine-specific medication included triptans or ergots.
Monthly averages are derived and normalized to 28 days equivalent by the following formula: (# days of efficacy variable over relevant period / # days with assessments recorded in the e-diary over the relevant period) * 28.
The change is calculated as postbaseline value - baseline value.
|
Baseline (Days -28 to Day -1), Treatment (Days 1 - Week 12)
|
Change From Baseline in the Number of Migraine Days During the 4 Week Period After the First Dose of Study Drug
Time Frame: Baseline (Days -28 to Day -1), Treatment (Days 1 - Week 4)
|
A migraine day was defined as when at least 1 of the following situations occurred: - a calendar day (0:00 to 23:59) demonstrating at least 4 consecutive hours of a headache endorsing criteria for migraine with or without aura - a calendar day (0:00 to 23:59) demonstrating at least 4 consecutive hours of a headache endorsing criteria for probable migraine, a migraine subtype where only 1 migraine criterion is missing - a calendar day (0:00 to 23:59) demonstrating a headache of any duration that was treated with migraine-specific medications (triptans and ergot compounds) Monthly averages are derived and normalized to 28 days equivalent by the following formula: (# days of efficacy variable over relevant period / # days with assessments recorded in the e-diary over the relevant period) * 28.
The change is calculated as postbaseline value - baseline value.
|
Baseline (Days -28 to Day -1), Treatment (Days 1 - Week 4)
|
Change From Baseline in the Monthly Average Number of Migraine Days During the 12 Week Period After the First Dose of Study Medication in Patients Not Receiving Concomitant Preventive Migraine Medications
Time Frame: Baseline (Days -28 to Day -1), Treatment (Days 1 - Week 12)
|
A subset of patients (specified in the protocol not to exceed 30%) were allowed to use 1 concomitant migraine preventive medication.
This outcome only includes those participants who did not take concomitant preventive migraine medication during this study.
A migraine day has been previously defined.
Monthly averages are derived and normalized to 28 days equivalent by the following formula: (# days of efficacy variable over relevant period / # days with assessments recorded in the e-diary over the relevant period) * 28.
The change is calculated as postbaseline value - baseline value.
|
Baseline (Days -28 to Day -1), Treatment (Days 1 - Week 12)
|
Change From Baseline in Migraine-Related Disability Score (MIDAS), As Measured by the Migraine Disability Assessment At 4 Weeks After the Last (3rd) Dose of Study Drug
Time Frame: Baseline (Day 0), Treatment Week 12 (4 weeks after the 3rd dose)
|
The MIDAS questionnaire is a 5-item instrument developed to assess headache-related disability based on lost days of activity in 3 domains (work, household work, and nonwork) over the previous 3 months.
The total score, ie, the sum of the # lost days answered for the first 5 questions, is used for grading of disability, with scores of 0-5 lost days = grade 1 (little or no disability), 6-10 lost days =grade 2 (mild disability), 11-20 lost days = grade 3 (moderate disability), and ≥21 lost days interpreted as grade 4 (severe disability).
Negative change from baseline scores indicate a reduction (improvement) in headache-related disability.
|
Baseline (Day 0), Treatment Week 12 (4 weeks after the 3rd dose)
|
Electrocardiogram Finding Shifts From Baseline to Overall
Time Frame: Baseline (Day 0), Treatment Week 12 (or early withdrawal)
|
12-lead ECGs were performed before other assessments (eg, blood draws and administration of questionnaires) and performed in triplicate.
The worst post-baseline finding for the patient is summarized.
Only patients with both baseline and post-baseline ECGs are included.
The ECG was evaluated by the investigator at the time of recording (signed and dated), and the printout was kept in the source documentation file.
When potentially clinically significant findings were detected by the investigator, a cardiologist at a central diagnostic center was consulted for a definitive interpretation.
Any ECG finding that was judged by the investigator as a potentially clinically significant change (worsening) compared with a baseline value was considered an adverse event.
- NCS = abnormal, not clinically significant - CS = abnormal, clinically significant Shift format is: baseline finding / worst post-baseline finding
|
Baseline (Day 0), Treatment Week 12 (or early withdrawal)
|
Participants With Vital Signs Potentially Clinically Significant Abnormal Values
Time Frame: Treatment Days 28, 56 and 84. Changes from previous reading may reflect the baseline reading performed on Day 0.
|
Vital signs were performed before other assessments (eg, blood draws and administration of questionnaires).
Vital signs with at least one participant showing potentially clinically significant abnormal findings included: - Pulse Rate Low: <=50 and decrease of >=15 beats per minute - Systolic Blood Pressure Low: <=90 mmHg and decrease of >=20 mmHg - Diastolic Blood Pressure High: >=105 mmHg and increase of >=15 mmHg - Diastolic Blood Pressure Low: <=50 mmHg and decrease of >=15 mmHg - Respiratory Rate Low: <10 breaths / minute
|
Treatment Days 28, 56 and 84. Changes from previous reading may reflect the baseline reading performed on Day 0.
|
Participants With Serum Chemistry and Hematology Potentially Clinically Significant Abnormal Results
Time Frame: Treatment Days 28, 56 and 84 (or early withdrawal)
|
Serum chemistry and hematology laboratory tests with potentially clinically significant abnormal findings included: - Blood Urea Nitrogen (BUN) High: >=10.71
mmol/L - Bilirubin High: >=34.2 umol/L - Alanine Aminotransferase (ALT): >=3*upper limit of normal (ULN) - Aspartate Aminotransferase (AST): >=3*upper limit of normal (ULN) - Gamma Glutamyl Transferase (GGT): >=3*upper limit of normal (ULN) - Hemoglobin: Male: <115 g/L or Female: <=95 g/L - Hematocrit: Male: <0.37 L/L or Female: <0.32 L/L - Leukocytes: >=20*10^9/L or <=3*10^9/L - Eosinophils/Leukocytes: >=10% - Platelets: >=700*10^9/L or <=75*10^9/L
|
Treatment Days 28, 56 and 84 (or early withdrawal)
|
Participants With Urinalysis Laboratory Tests Potentially Clinically Significant Abnormal Results
Time Frame: Treatment Days 28, 56 and 84. Changes from previous reading reflect the baseline reading performed on Day 0.
|
Urinalysis with potentially clinically significant abnormal findings included: - Blood: >=2 unit increase from baseline - Urine Glucose (mg/dL): >=2 unit increase from baseline - Ketones (mg/dL): >=2 unit increase from baseline - Urine Protein (mg/dL): >=2 unit increase from baseline
|
Treatment Days 28, 56 and 84. Changes from previous reading reflect the baseline reading performed on Day 0.
|
Participants With Positive Electronic Columbia Suicide Severity Rating Scale Results After the First Dose of Study Drug
Time Frame: Day 1 to Week 12
|
The electronic Columbia-Suicide Severity Rating Scale (eC-SSRS) was used to assess the patient's suicidal ideation (severity and intensity) and behavior (Posner et al 2011).
The eC-SSRS Baseline/Screening version was completed by the patient at visit 2, and the eC-SSRS Since Last Visit version was completed by the patient at all other time points.
Any positive findings on the eC-SSRS Since Last Visit version required evaluation by a physician or doctoral-level psychologist.
Findings after the first dose of study drug using the eC-SSRS Since Last Visit version are summarized.
|
Day 1 to Week 12
|
Collaborators and Investigators
Publications and helpful links
General Publications
- McAllister P, Cohen JM, Campos VR, Ning X, Janka L, Barash S. Impact of fremanezumab on disability outcomes in patients with episodic and chronic migraine: a pooled analysis of phase 3 studies. J Headache Pain. 2022 Aug 29;23(1):112. doi: 10.1186/s10194-022-01438-4.
- Diener HC, McAllister P, Jurgens TP, Kessler Y, Ning X, Cohen JM, Campos VR, Barash S, Silberstein SD. Safety and tolerability of fremanezumab in patients with episodic and chronic migraine: a pooled analysis of phase 3 studies. Cephalalgia. 2022 Jul;42(8):769-780. doi: 10.1177/03331024221076485. Epub 2022 Mar 25.
- Nahas SJ, Naegel S, Cohen JM, Ning X, Janka L, Campos VR, Krasenbaum LJ, Holle-Lee D, Kudrow D, Lampl C. Efficacy and safety of fremanezumab in clinical trial participants aged >/=60 years with episodic or chronic migraine: pooled results from 3 randomized, double-blind, placebo-controlled phase 3 studies. J Headache Pain. 2021 Nov 24;22(1):141. doi: 10.1186/s10194-021-01351-2. Erratum In: J Headache Pain. 2022 May 17;23(1):57.
- Silberstein SD, Cohen JM, Yang R, Gandhi SK, Du E, Jann AE, Marmura MJ. Treatment benefit among migraine patients taking fremanezumab: results from a post hoc responder analysis of two placebo-controlled trials. J Headache Pain. 2021 Jan 7;22(1):2. doi: 10.1186/s10194-020-01212-4.
- Brandes JL, Kudrow D, Yeung PP, Sakai F, Aycardi E, Blankenbiller T, Grozinski-Wolff M, Yang R, Ma Y. Effects of fremanezumab on the use of acute headache medication and associated symptoms of migraine in patients with episodic migraine. Cephalalgia. 2020 Apr;40(5):470-477. doi: 10.1177/0333102419885905. Epub 2019 Nov 21.
- Dodick DW, Silberstein SD, Bigal ME, Yeung PP, Goadsby PJ, Blankenbiller T, Grozinski-Wolff M, Yang R, Ma Y, Aycardi E. Effect of Fremanezumab Compared With Placebo for Prevention of Episodic Migraine: A Randomized Clinical Trial. JAMA. 2018 May 15;319(19):1999-2008. doi: 10.1001/jama.2018.4853.
Study record dates
Study Major Dates
Study Start (Actual)
Primary Completion (Actual)
Study Completion (Actual)
Study Registration Dates
First Submitted
First Submitted That Met QC Criteria
First Posted (Estimate)
Study Record Updates
Last Update Posted (Actual)
Last Update Submitted That Met QC Criteria
Last Verified
More Information
Terms related to this study
Additional Relevant MeSH Terms
- Brain Diseases
- Central Nervous System Diseases
- Nervous System Diseases
- Headache Disorders, Primary
- Headache Disorders
- Migraine Disorders
- Physiological Effects of Drugs
- Vasodilator Agents
- Bone Density Conservation Agents
- Calcium-Regulating Hormones and Agents
- Calcitonin
- Calcitonin Gene-Related Peptide
- Katacalcin
Other Study ID Numbers
- TV48125-CNS-30050
- 2015-004598-34 (EudraCT Number)
Drug and device information, study documents
Studies a U.S. FDA-regulated drug product
Studies a U.S. FDA-regulated device product
This information was retrieved directly from the website clinicaltrials.gov without any changes. If you have any requests to change, remove or update your study details, please contact register@clinicaltrials.gov. As soon as a change is implemented on clinicaltrials.gov, this will be updated automatically on our website as well.
Clinical Trials on Migraine
-
Austrian Migraine Registry CollaborationMedical University of Vienna; Medical University Innsbruck; Austrian Headache...RecruitingMigraine | Chronic Migraine | Migraine Without Aura | Migraine With Aura | Episodic MigraineAustria
-
Tonix Pharmaceuticals, Inc.PremierCompletedChronic Migraine | Chronic Migraine, Headache | Chronic Migraine Without Aura | Aura MigraineUnited States
-
Harvard University Faculty of MedicineBrigham and Women's Hospital; Palmer Center for Chiropractic Research (PCCR)CompletedMigraine | Migraine Disorders | Migraine Without Aura | Migraine With Aura | Migraine, ClassicUnited States
-
University of FlorenceAzienda Ospedaliera Città della Salute e della Scienza di Torino; University... and other collaboratorsRecruitingMigraine | Chronic Migraine | Migraine Without Aura | Migraine With AuraItaly
-
CoolTech LLCTerminatedMigraine | Migraine Without Aura | Migraine With Aura | Episodic MigraineUnited States
-
University of FlorenceAzienda Ospedaliera Città della Salute e della Scienza di Torino; University... and other collaboratorsRecruitingMigraine | Chronic Migraine | Migraine Without Aura | Migraine With AuraItaly
-
Notre-Dame Hospital, Montreal, Quebec, CanadaAllerganCompletedChronic Migraine | Migraine Without Aura | Migraine With AuraCanada
-
Glostrup University Hospital, CopenhagenUnknownChronic Migraine | Migraine Without Aura | Migraine With AuraDenmark
-
Fondazione I.R.C.C.S. Istituto Neurologico Carlo...CompletedMigraine With Aura | Migraine in ChildrenItaly
-
The Cleveland ClinicWithdrawnMigraine | Migraine Disorders | Headache Disorders, Primary | Migraine Headache | Migraine Without Aura | Migraine With Aura | Headache, MigraineUnited States
Clinical Trials on Placebo
-
SamA Pharmaceutical Co., LtdUnknownAcute Bronchitis | Acute Upper Respiratory Tract InfectionKorea, Republic of
-
National Institute on Drug Abuse (NIDA)CompletedCannabis UseUnited States
-
AstraZenecaParexel; Spandauer Damm 130; 14050; Berlin, GermanyCompletedMale Subjects With Type II Diabetes (T2DM)Germany
-
Heptares Therapeutics LimitedCompletedPharmacokinetics | Safety IssuesUnited Kingdom
-
GlaxoSmithKlineCompletedPulmonary Disease, Chronic ObstructiveUnited Kingdom, Netherlands
-
ItalfarmacoCompletedBecker Muscular DystrophyNetherlands, Italy
-
Shijiazhuang Yiling Pharmaceutical Co. LtdXuanwu Hospital, BeijingCompleted
-
GlaxoSmithKlineCompletedInfections, BacterialUnited States
-
West Penn Allegheny Health SystemCompletedAsthma | Allergic RhinitisUnited States