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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT02891226
Other study ID # 16492
Secondary ID I6T-MC-AMAG2016-
Status Completed
Phase Phase 2
First received
Last updated
Start date December 14, 2016
Est. completion date February 5, 2021

Study information

Verified date August 2022
Source Eli Lilly and Company
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

The purpose of this study is to evaluate the safety and effectiveness of the study drug Mirikizumab in participants with active Crohn's Disease.


Recruitment information / eligibility

Status Completed
Enrollment 191
Est. completion date February 5, 2021
Est. primary completion date December 11, 2018
Accepts healthy volunteers No
Gender All
Age group 18 Years to 75 Years
Eligibility Inclusion Criteria: - Active Crohn's Disease (CD) as determined by the SES-CD, and participant reported stool frequency and abdominal pain. - Inadequate response or failure to tolerate at least one of the following: aminosalicylates; budesonide; systemic corticosteroids; immunosuppressants (eg, azathioprine, 6-mercaptopurine, or methotrexate); or prior exposure to biologics for the treatment of CD. Exclusion Criteria: - Have complications of CD such as strictures, stenoses, or any other manifestation for which surgery might be indicated, or that could confound the evaluation of efficacy. - Diagnosis of conditions affecting the digestive tract, such as ulcerative colitis, indeterminate colitis, fistulizing disease, abdominal or perianal abscess, adenomatous colonic polyps not excised, colonic mucosal dysplasia, and short bowel syndrome. - Have had any kind of bowel resection, diversion, or placement of a stoma within 6 months or any other intra-abdominal surgery within 3 months prior to screening. - Are unsuitable for inclusion in the study in the opinion of the investigator or sponsor for any reason that may compromise the subject's safety or confound data interpretation.

Study Design


Related Conditions & MeSH terms


Intervention

Drug:
Mirikizumab

Placebo


Locations

Country Name City State
Australia Royal Adelaide Hospital Adelaide South Australia
Australia Ballarat Health Services - Base Hospital Ballarat Victoria
Australia St Vincents Hospital Melbourne Fitzroy Victoria
Australia Princess Alexandra Hospital Woolloongabba Queensland
Belgium Hospital Universitaire Erasme Brussel Brussel
Belgium Universitair Ziekenhuis Gent Gent
Canada Sudbury Endoscopy Centre Sudbury Ontario
Czechia Hepato-gastroenterologie HK, s.r.o. Hradec Kralove
Czechia Gregar s.r.o. Olomouc
Czechia Thomayerova Nemocnice Praha 4 - Krc
Czechia Fakultni Nemocnice v Motole Praha 5
Czechia Krajska zdravotni a.s. - Masarykova nemocnice v Usti nad Labem, o.z. Usti nad Labem Czech Republic
Czechia Krajska nemocnice T. Bati a.s. Zlin
Hungary Obudai Egeszsegugyi Centrum Kft Budapest
Hungary Javorszky Odon Hospital Vac
Japan Tokyo Medical And Dental University Hospital Bunkyo-ku Tokyo
Japan Fukuoka University Chikushi Hospital Chikushino-shi Fukuoka-Ken
Japan Fukuoka University Hospital Fukuoka
Japan Sameshima Hospital Kagoshima-shi Kagoshima
Japan Gokeikai Ofuna Chuo Hospital Kamakura-shi Kanagawa
Japan Kitakyushu Municipal Medical Center Kitakyusyu-shi Fukoka
Japan Kyorin University Hospital Mitaka Tokyo
Japan Kinshukai Infusion Clinic Osaka-shi Osaka-Fu
Japan Toho University School of Medicine, Sakura Hospital Sakura-shi Chiba-Ken
Japan Hokkaido P.W.F.A.C. Sapporo-Kosei General Hospital Sapporo-shi Hokkaido
Japan Takagi Clinic Sendai-shi Miyagi-Ken
Japan JHCO Tokyo Yamate Medical Center Shinjuku-ku Tokyo
Japan Toyama Prefectural Central Hospital Toyama-Shi Toyama
Netherlands Academisch Medisch Centrum Amsterdam
Netherlands Radboud Universitair Medisch Centrum Nijmegen Nijmegen
Netherlands Erasmus Medisch Centrum Rotterdam
Netherlands St Elisabeth Ziekenhuis Tilburg Noord Brabant
Poland Szpital Uniwersytecki nr 2 im. dr J. Biziela Bydgoszcz
Poland KO-MED Centra Kliniczne Lublin II Lublin
Poland SOLUMED Centrum Medyczne Poznan
Poland Korczowski Bartosz, Gabinet Lekarski Rzeszow
Poland Twoja Przychodnia-Szczecinskie Centrum Medyczne Szczecin
Poland Centrum Zdrowia Matki, Dziecka i Mlodziezy Warszawa
Poland Melita Medical Sp. Z O. O. Wroclaw
Romania SC Med Life SA Bucuresti
Romania SC Pelican SRL Oradea Bihor
Romania S.C Centrul de Gastroenterologie Dr. Goldis S.R.L Timisoara
Russian Federation FSBI Scientific Research Inst. of Physyology and Basic Medic Novosibirsk
Russian Federation Novosibirsk State Medical University Novosibirsk
Russian Federation Ultramed Omsk
Russian Federation City Clinical Hospital # 2 n.a. Fedor Khristoforovich Gral Perm
Russian Federation Private Medical Institution Evromedservis Pushkin
Russian Federation Medical Institute REAVIZ Samara
Russian Federation NonState Healthcare Institution Central Clinical Hospital Samara
Russian Federation Baltic Medicine St. Petersburg
Russian Federation City Hospital of Saint Martyr Elizabeth St. Petersburg
Russian Federation LLC Scientific Research Centre EKO-Bezopasnost St. Petersburg
Russian Federation Ulyanovsk Regional Clinical Hospital Ulyanovsk
Switzerland Universitätsspital Zürich Zürich
Ukraine Communal institution of the Kyiv Regional Council "Kyiv Regional Clinical Oncology Dispensary" Kyiv
Ukraine Kyiv Municipal Clinical Hospital #1 Kyiv
Ukraine Lviv Regional Central Hospital Lviv
Ukraine Odesa Regional Clinical Hospital Odesa
Ukraine A. Novak Transcarpathian Regional Clinical Hospital Uzhgorod
Ukraine SRI of Invalid Rehabil.,Educ.Scient.Med.Complex Vinnytsia
Ukraine Vinnitsa City Clinical Hospital #1 Vinnytsya
Ukraine CI City Hospital #1 Zaporizhzhia
Ukraine City Clinical Hospital #6 Zaporizhzhia
United Kingdom Queen Elizabeth University Hospital Glasgow
United States University of Michigan Health Systems Ann Arbor Michigan
United States Texas Clinical Research Institute, LLC Arlington Texas
United States Digestive Healthcare of Georgia Atlanta Georgia
United States University of North Carolina Chapel Hill North Carolina
United States Consultants For Clinical Research Cincinnati Ohio
United States Clinical Research of West Florida Clearwater Florida
United States University Hospitals Health Center Cleveland Ohio
United States Delta Waves Sleep Disorders and Research Center Colorado Springs Colorado
United States Columbus Regional Research Institute Columbus Georgia
United States Valley View Internal Medicine Garden Grove California
United States Gastro One Germantown Tennessee
United States NYU Langone Long Island Clinical Research Associates Great Neck New York
United States Carolina Digestive Diseases Greenville North Carolina
United States Medical Research Center of Connecticut Hamden Connecticut
United States Wellness Clinical Research Hialeah Gardens Florida
United States Hermann Drive Surgical Hospital Houston Texas
United States Longwood Research Huntsville Alabama
United States Indiana University Health Indianapolis Indiana
United States Las Vegas Medical Research Las Vegas Nevada
United States Ocean State Clinical Research Partners Lincoln Rhode Island
United States Robley Rex VAMC Louisville Kentucky
United States University of Miami Miami Florida
United States Vista Health Research Miami Florida
United States Delta Research Partners LLC Monroe Louisiana
United States Columbia University Medical Center New York New York
United States University of Oklahoma Health Sciences Center Oklahoma City Oklahoma
United States Clinical Neuroscience Solutions Inc Orlando Florida
United States Health Quest Medical Care Owensboro Kentucky
United States Minnesota Gastroenterology, P.A. Plymouth Minnesota
United States Digestive Health Associates of Texas Richardson Texas
United States MedStar Health Research Institute Rosedale Maryland
United States St. Louis Center for Clinical Research Saint Louis Missouri
United States Washington University Medical School Saint Louis Missouri
United States Care Access Research - Salt Lake City Salt Lake City Utah
United States San Antonio Gastroenterology San Antonio Texas
United States University of Washington Medical Center Seattle Washington
United States Virginia Mason Medical Center Seattle Washington
United States Louisiana Research Center Shreveport Louisiana
United States Holy Name Medical Center Teaneck New Jersey
United States Del Sol Research Management, LLC Tucson Arizona
United States Healthcare Research Consultant Tulsa Oklahoma
United States Advanced Gastroenterology Union City Tennessee
United States Ventura Clinical Trials Ventura California
United States Huron Gastroenterology Associates Ypsilanti Michigan

Sponsors (1)

Lead Sponsor Collaborator
Eli Lilly and Company

Countries where clinical trial is conducted

United States,  Australia,  Belgium,  Canada,  Czechia,  Hungary,  Japan,  Netherlands,  Poland,  Romania,  Russian Federation,  Switzerland,  Ukraine,  United Kingdom, 

Outcome

Type Measure Description Time frame Safety issue
Primary Percentage of Participants Achieving Endoscopic Response at Week 12 Endoscopic response defined as = 50% reduction from baseline in Simple Endoscopic Score for Crohn's Disease (SES-CD) at Week 12. The SES-CD evaluates 4 endoscopic variables: presence and size of ulcers, proportion of surface covered by ulcers, proportion of surface affected by disease, and presence and severity of stenosis. The total SES-CD calculated as sum of 4 variables for 5 bowel segments: (ileum;right,transverse,and left colon;and rectum): presence and size of ulcers (none = score 0; diameter 0.1-0.5 cm = score 1; 0.5-2 cm = score 2; >2 cm = score 3); extent of ulcerated surface (none = 0; <10% = 1;10-30% = 2;>30% = 3);extent of affected surface (none = 0; <50% = 1;50-75% = 2;>75% =3); and presence and type of narrowings (none=0; single, can be passed=1; multiple,can be passed=2; cannot be passed=3). Total SES-CD scores range from 0 to 56, with higher scores indicating more severe disease. Week 12
Secondary Percentage of Participants Achieving Endoscopic Remission at Week 12 Endoscopic remission defined as SES-CD of <4 ileal-colonic or <2 for isolated ileal disease, and no subscore >1 at week 12. The SES-CD evaluates 4 endoscopic variables: presence and size of ulcers, proportion of surface covered by ulcers, proportion of surface affected by disease, and presence and severity of stenosis. The total SES-CD is calculated as the sum of the 4 variables for the 5 bowel segments: (ileum; right, transverse, and left colon; and rectum): presence and size of ulcers (none = score 0; diameter 0.1-0.5 cm = score 1; 0.5-2 cm = score 2; greater than (>) 2 cm = score 3); extent of ulcerated surface (none = 0; less than (<) 10% = 1; 10-30% = 2; >30% = 3); extent of affected surface (none = 0; <50% = 1; 50-75% = 2; >75% = 3); and presence and type of narrowings (none=0; single, can be passed=1; multiple, can be passed=2; cannot be passed=3). Total SES-CD scores range from 0 to 56, with higher scores indicating more severe disease. Week 12
Secondary Percentage of Participants Achieving Patient Reported Outcome Remission at Week 12 PRO remission is defined as stool frequency (SF) =2.5 and abdominal pain (AP) =1 and no worse than baseline at week 12. SF captures the number of liquid or very soft stools. AP score is classified as 0=none, 1=mild, 2=moderate, 3=severe. Week 12
Secondary Mean Change From Baseline on the Patient Global Rating - Severity (PGRS) Crohn's Disease Score at Week 12 The PGRS is a 1-item patient-rated questionnaire designed to assess the participant's rating of their disease symptom severity over the past 24 hours. Responses are graded on a 6-point scale in which a score of 1 indicates the subject has no symptoms (that is, "none") and a score of 6 indicates that the participant's symptom are "very severe." Least Squares Mean (LS Mean) was calculated using Mixed Model for Repeated Measures (MMRM) model with treatment, geographic region, geographic region, prior biologic CD therapy use (prior biologic experience versus prior biologic naive), baseline score, visit, and the interaction of treatment-by-visit and baseline-by-visit as fixed factors. Baseline, Week 12
Secondary Mean of Patient Global Rating - Change (PGRC) Crohn's Disease Score at Week 12 The PGRC scale is a patient-rated instrument designed to assess the participant's rating of change in their symptom(s). Responses are graded on a 7-point Likert scale in which a score of 1 indicates that the participant's symptom is "very much better," a score of 4 indicates that the participant's symptom has experienced "no change," and a score of 7 indicates that the participant's symptom is "very much worse." Baseline, Week 12
Secondary Mean Change From Baseline on the Inflammatory Bowel Disease Questionnaire (IBDQ) Score at Week 12 The IBDQ is a 32-item self-administered questionnaire. The IBDQ has 4 dimensions: bowel symptoms (10 items), systemic symptoms (5 items), emotional function (12 items), and social function (5 items). Responses are graded on a 7-point Likert scale in which 7 denotes "not a problem at all" and 1 denotes "a very severe problem." Scores range from 32 to 224; a higher score indicates a better quality of life. LS Mean was calculated using Mixed Model for Repeated Measures (MMRM) model with treatment, geographic region, geographic region, prior biologic CD therapy use (prior biologic experience versus prior biologic naive), baseline score, visit, and the interaction of treatment-by-visit and baseline-by-visit as fixed factors. Baseline, Week 12
Secondary Mean Change From Baseline on the Functional Assessment of Chronic Illness Therapy-Fatigue (FACIT-F) Score at Week 12 The Functional Assessment of Chronic Illness Therapy-Fatigue (FACIT-F) Scale is a13-item, symptom-specific questionnaire that specifically assesses the participant's self-reported severity of fatigue and its impact upon daily activities and functioning. The FACIT-F uses a numeric rating scale of 0-4 associated with a range over "Not at all" to "Very much" for each item to assess fatigue and its impact in the past 7 days. Total scores range from 0 to 52, with higher scores indicating less fatigue. LS Mean was calculated using Mixed Model for Repeated Measures (MMRM) model with treatment, geographic region, geographic region, prior biologic CD therapy use (prior biologic experience versus prior biologic naive), baseline score, visit, and the interaction of treatment-by-visit and baseline-by-visit as fixed factors. Baseline, Week 12
Secondary Mean Change From Baseline on the 36-Item Short Form Health Survey (SF-36) Physical Component Summary (PCS) and Mental Component Summary (MCS) Scores at Week 12 The SF-36 is a health-related survey that assesses participant's quality of life and consists of 36 questions covering 8 health domains:physical functioning, bodily pain, role limitations due to physical problems and emotional problems, general health, mental health, social functioning, vitality, 2 component scores (MCS and PCS). MCS consisted of social functioning, vitality, mental health, and role-emotional scales. PCS consisted of physical functioning, bodily pain, role-physical, and general health scales. Each domain is scored by summing individual items and transforming scores into a 0 to 100 scale with higher scores indicating better health status or functioning. LS Mean was calculated using Mixed Model for Repeated Measures (MMRM) model with treatment, geographic region, geographic region, prior biologic CD therapy use (prior biologic experience versus prior biologic naive), baseline score, visit, and the interaction of treatment-by-visit and baseline-by-visit as fixed factors. Baseline, Week 12
Secondary Population Pharmacokinetics (PopPK): Mean Population Clearance of Mirikizumab Population mean (between-subject coefficient variance [CV %]) apparent clearance. Clearance is estimated based on concentration data collected in the time frame of 0-208 weeks. Week 0, 4, 8: Predose, end of infusion; Week 2; 4; 6; 8, 11-12; 12-13; 16; 20; 24; 28; 36; 44; 52; 60; 68; 76; 84; 92; 104; 108; 112; 120; 128; 136; 144; 156; 164; 172; 180; 188; 196 and 208 weeks post infusion
Secondary Population Pharmacokinetics (PopPK): Mean Population Volume of Distribution of Mirikizumab Population mean (between-subject coefficient variance [CV %]) apparent volume of distribution. Volume of distribution is estimated based on concentration data collected in the time frame of 0-208 weeks. Week 0, 4, 8: Predose, end of infusion; Week 2; 4; 6; 8, 11-12; 12-13; 16; 20; 24; 28; 36; 44; 52; 60; 68; 76; 84; 92; 104; 108; 112; 120; 128; 136; 144; 156; 164; 172; 180; 188; 196 and 208 weeks post infusion
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