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NCT01277666 Clinical Trial

A Study to Investigate the Efficacy and Safety of GSK1605786A in the Treatment of Subjects With Moderately-to-Severely Active Crohn's Disease

Crohn's Disease Clinical Trial

SHIELD-1

Official title:
A Randomised, Double-Blind, Placebo-Controlled Study to Investigate the Efficacy and Safety of GSK1605786A in the Treatment of Subjects With Moderately-to-Severely Active Crohn's Disease

Clinical Trial Details — Status: Completed

Administrative data
NCT number NCT01277666
Other study ID # 114151
Secondary ID
Status Completed
Phase Phase 3
First received January 13, 2011
Last updated August 21, 2017
Start date December 20, 2010
Est. completion date July 11, 2013

Study information
Verified date July 2017
Source GlaxoSmithKline
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

This is a randomised, double-blind, placebo-controlled study to evaluate the efficacy and safety of two doses (500 mg once daily and 500 mg twice daily) of GSK1605786A as compared to placebo over 12 weeks in adult subjects with moderately-to-severely active Crohn's disease. Efficacy will be assessed by proportion of subjects achieving response, defined as a decrease in Crohn's Disease Activity Index (CDAI) score of at least 100 points (clinical response). Clinical remission (CDAI score less than 150 points) will be evaluated as a key secondary endpoint. Safety will be assessed by recording of adverse events, clinical laboratory parameters, vital signs and electrocardiogram (ECG). Population pharmacokinetics will evaluate the two doses of GSK1605786A. Health outcomes assessments will include changes in Inflammatory Bowel Disease Questionnaire (IBDQ), Short Form-36 version 2 (SF-36v2), EQ-5D and Work Productivity and Activity Impairment-CD (WPAI-CD) and receipt of disability.

Description:

This is a multi-centre, randomised, double-blind, placebo-controlled, parallel group study to evaluate the efficacy of two oral doses of GSK1605786A (500 mg once daily, 500 mg twice daily) as compared to placebo in the induction of clinical response over a 12-week treatment period in subjects with moderately-to-severely active Crohn's disease. Secondary objectives will include assessment of the safety and evaluation of the efficacy in induction of remission.

The study is planned to randomise approximately 600 subjects (200 subjects/group) with active Crohn's disease, diagnosed for at least 4 months with a documented history of disease in the small and/or large intestine, and characterised by a Crohn's Disease Activity Index (CDAI) score between 220 to and 450, inclusive. Subjects must have reported an inadequate response or intolerance to Crohn's disease treatment with corticosteroids or immunosuppressants. Inclusion of subjects who received prior treatment with a biologic anti-tumour necrosis factor (TNF) agent will be limited to approximately 50% of the study population. All subjects are required to have a diagnosis with identification of anatomic location of Crohn's disease, which has been established by visualisation of the gastrointestinal tract within 12 months of screening. Subjects who have not had a visualisation of the gastrointestinal tract within 12 months are required to undergo an endoscopic assessment during the screening period. Subjects will be required to have evidence of current active inflammation at the time of randomisation either by endoscopy or by inflammatory biomarkers [elevated C-reactive protein (CRP) greater than the upper limit of normal (ULN) plus a positive faecal calprotectin test]. Subjects who do not meet the requirements based on inflammatory biomarker test results will be required to qualify based on endoscopic assessment during screening. Subjects will be allowed to participate in the study while continuing on stable doses of agents typically used to treat Crohn's disease. Following the screening period, subjects will be randomised at baseline to receive blinded treatment with one of two doses of GSK1605786A (500 mg once daily or twice daily) or placebo for 12 weeks. Response and remission endpoints, using the CDAI, will be evaluated at Weeks 4, 8 and 12.

Recruitment information / eligibility
Status Completed
Enrollment 608
Est. completion date July 11, 2013
Est. primary completion date July 11, 2013
Accepts healthy volunteers No
Gender All
Age group 18 Years and older
Eligibility Inclusion Criteria:

- Male or female subjects aged 18 years or older

- Written informed consent

- Diagnosis of Crohn's disease for greater than 4 months duration with small bowel and/or colonic involvement

- Confirmation of Crohn's disease established by visualisation of the gastrointestinal tract within the 12 months prior to screening or by screening endoscopy at study entry

- History of inadequate response and/or intolerance/adverse event leading to discontinuation of either corticosteroids or immunosuppressants

- Moderately-to-severely active disease characterised by a CDAI score between 220 and 450, inclusive, at Baseline

- Confirmation of current active Crohn's disease by screening endoscopy or inflammatory biomarkers [elevated C-reactive protein (greater than upper limit of normal) plus positive test for faecal calprotectin] at Screening

- Stable doses of permitted concomitant medications or having previously received, but are not currently receiving, medications for Crohn's disease

- Demonstrated ability to comply with Crohn's disease symptom recording using the interactive voice response system

- Females of child-bearing potential must be sexually inactive or commit to consistent and correct use of a contraceptive method of birth control with a failure rate of less than 1% for the duration of this study

Exclusion Criteria:

- If female: pregnant, has a positive pregnancy test or is breast-feeding

- Diagnosis of coeliac disease, follow a gluten-free diet to manage symptoms, or positive test for coeliac disease

- Diagnosis of ulcerative or indeterminate colitis

- Enterocutaneous, abdominal or pelvic fistulae with abscesses or fistulae likely to require surgery during the study period

- Bowel surgery, other than appendectomy, within 12 weeks prior to screen and/or has surgery planned or deemed likely for Crohn's disease during the study period

- Extensive colonic resection, subtotal or total colectomy

- Presence of ileostomies, colostomies or rectal pouches

- Known fixed symptomatic stenoses

- History of more than 3 small bowel resections or diagnosis of short bowel syndrome

- Chronic use of narcotics for chronic pain defined as daily use of one or more doses of narcotic containing medication

- Use of prohibited medications, including enteral feeding or elemental diet, within their specified time frames

1. Biologic use: Use of any biologic (tumour necrosis factor inhibitor or natalizumab) within 8 weeks prior to screening

2. Corticosteroid use: Use of parenteral glucocorticoids within 4 weeks prior to screening

3. Immunospressant use: Use of cyclosporine, tacrolimus, sirolimus or mycophenolate mofetil within 4 weeks prior to screening

4. Intravenous antibiotic use: Use of intravenous antibiotics for Crohn's disease within 4 weeks prior to screening

5. Use of rectal treatment with 5-ASA or corticosteroid enemas/suppositories within 2 weeks prior to screening

6. Use of tube or enteral feeding, elemental diet, or parenteral alimentation within 2 weeks prior to screening

7. Leukocytapheresis or granulocytapheresis within 2 weeks prior to screening

- Positive immunoassay for Clostridium difficile

- Known human immunodeficiency virus (HIV) infection

- Known varicella, herpes zoster, or other severe viral infection within 6 weeks of screening

- Immunisation with a live vaccine within 4 weeks of screening, with the exception of influenza vaccine

- Active or latent tuberculosis infection

- Current sepsis or infections requiring intravenous antibiotic therapy for more than 2 weeks

- Evidence of hepatic dysfunction, viral hepatitis, or current or chronic history of liver disease including non-alcoholic steatohepatitis (NASH)

- Positive test for Hepatitis B or Hepatitis C antibody at screening

- Corrected QT interval of ECG (electrocardiogram) greater than or equal to 450 milliseconds

- Concurrent illness or disability that may affect the interpretation of clinical data, or otherwise contraindicates participation in this clinical study

- History or evidence of adenomatous colonic polyps that have not been removed

- History of evidence of colonic mucosal dysplasia

- Current evidence of, or has been treated for a malignancy within the past five years (other than localised basal cell, squamous cell skin cancer, cervical dysplasia, or any cancer in situ that has been resected)

- Any previous participation in a clinical study of GSK1605786A (formerly ChemoCentryx compound CCX282-B)

- Medical history of sensitivity to any of the components of GSK1605786A

- Use of any investigational product within 30 days prior to screening

Study Design

Related Conditions & MeSH terms

Intervention

Drug:
GSK1605786A
500 mg twice daily, administered orally for 12 weeks
GSK1605786A
500 mg once daily, administered orally for 12 weeks
Placebo
Placebo capsules, administered orally for 12 weeks

Locations
Country Name City State
Australia GSK Investigational Site Adelaide South Australia
Australia GSK Investigational Site Bankstown New South Wales
Australia GSK Investigational Site Fitzroy Victoria
Australia GSK Investigational Site Fremantle Western Australia
Australia GSK Investigational Site Hersten Queensland
Australia GSK Investigational Site Kurralta Park South Australia
Australia GSK Investigational Site Prahran Victoria
Austria GSK Investigational Site Hall in Tirol
Austria GSK Investigational Site Linz
Austria GSK Investigational Site Wien
Austria GSK Investigational Site Wien
Belgium GSK Investigational Site Bonheiden
Belgium GSK Investigational Site Brussels
Belgium GSK Investigational Site Brussels
Belgium GSK Investigational Site Edegem
Belgium GSK Investigational Site Gent
Belgium GSK Investigational Site Kortrijk
Belgium GSK Investigational Site Leuven
Belgium GSK Investigational Site Roeselare
Canada GSK Investigational Site Abbotsford British Columbia
Canada GSK Investigational Site Calgary Alberta
Canada GSK Investigational Site Edmonton Alberta
Canada GSK Investigational Site Halifax Nova Scotia
Canada GSK Investigational Site Hamilton Ontario
Canada GSK Investigational Site Hamilton Ontario
Canada GSK Investigational Site Kingston Ontario
Canada GSK Investigational Site Levis Quebec
Canada GSK Investigational Site London Ontario
Canada GSK Investigational Site London Ontario
Canada GSK Investigational Site Montreal Quebec
Canada GSK Investigational Site Montreal Quebec
Canada GSK Investigational Site Ottawa Ontario
Canada GSK Investigational Site Quebec
Canada GSK Investigational Site Quebec
Canada GSK Investigational Site Richmond Hill Ontario
Canada GSK Investigational Site Toronto Ontario
Canada GSK Investigational Site Vancouver British Columbia
Canada GSK Investigational Site Victoria British Columbia
Canada GSK Investigational Site Winnipeg Manitoba
Czechia GSK Investigational Site Brno
Czechia GSK Investigational Site Hradec Králové
Czechia GSK Investigational Site Olomouc
Czechia GSK Investigational Site Ostrava - Vitkovice
Czechia GSK Investigational Site Praha 10
Czechia GSK Investigational Site Praha 4
Czechia GSK Investigational Site Praha 7
Czechia GSK Investigational Site Praha 9
Denmark GSK Investigational Site Aalborg
Denmark GSK Investigational Site Aarhus
Denmark GSK Investigational Site Herlev
Denmark GSK Investigational Site Hvidovre
Denmark GSK Investigational Site Odense
France GSK Investigational Site Amiens cedex 1
France GSK Investigational Site Clichy cedex
France GSK Investigational Site Lille cedex
France GSK Investigational Site Nantes cedex 1
France GSK Investigational Site Nice cedex 3
France GSK Investigational Site Paris cedex 10
France GSK Investigational Site Pessac cedex
France GSK Investigational Site Saint-Priest en Jarez
France GSK Investigational Site Vandoeuvre Les Nancy
Germany GSK Investigational Site Berlin
Germany GSK Investigational Site Berlin
Germany GSK Investigational Site Berlin
Germany GSK Investigational Site Braunschweig Niedersachsen
Germany GSK Investigational Site Brinkum/Stuhr Niedersachsen
Germany GSK Investigational Site Dessau Sachsen-Anhalt
Germany GSK Investigational Site Frankfurt am Main Hessen
Germany GSK Investigational Site Freiburg Baden-Wuerttemberg
Germany GSK Investigational Site Halle Sachsen-Anhalt
Germany GSK Investigational Site Hamburg
Germany GSK Investigational Site Hamburg
Germany GSK Investigational Site Hannover Niedersachsen
Germany GSK Investigational Site Jena Thueringen
Germany GSK Investigational Site Koeln Nordrhein-Westfalen
Germany GSK Investigational Site Ludwigshafen Rheinland-Pfalz
Germany GSK Investigational Site Minden Nordrhein-Westfalen
Germany GSK Investigational Site Muenster Nordrhein-Westfalen
Germany GSK Investigational Site Muenster Nordrhein-Westfalen
Germany GSK Investigational Site Ulm Baden-Wuerttemberg
Hungary GSK Investigational Site Bekescsaba
Hungary GSK Investigational Site Budapest
Hungary GSK Investigational Site Szekszárd
Israel GSK Investigational Site Haifa
Israel GSK Investigational Site Holon
Israel GSK Investigational Site Jerusalem
Israel GSK Investigational Site Jerusalem
Israel GSK Investigational Site Kfar Saba
Israel GSK Investigational Site Petach Tikva
Israel GSK Investigational Site Tel Aviv
Italy GSK Investigational Site Genova
Italy GSK Investigational Site Modena
Italy GSK Investigational Site Palermo Sicilia
Italy GSK Investigational Site Roma
Italy GSK Investigational Site Roma
Japan GSK Investigational Site Aichi
Japan GSK Investigational Site Aichi
Japan GSK Investigational Site Chiba
Japan GSK Investigational Site Fukuoka
Japan GSK Investigational Site Fukuoka
Japan GSK Investigational Site Hokkaido
Japan GSK Investigational Site Hyogo
Japan GSK Investigational Site Kagoshima
Japan GSK Investigational Site Kagoshima
Japan GSK Investigational Site Miyagi
Japan GSK Investigational Site Osaka
Japan GSK Investigational Site Osaka
Japan GSK Investigational Site Tokyo
Japan GSK Investigational Site Tokyo
Japan GSK Investigational Site Tokyo
Korea, Republic of GSK Investigational Site Daegu
Korea, Republic of GSK Investigational Site Pusan
Korea, Republic of GSK Investigational Site Seoul
Korea, Republic of GSK Investigational Site Seoul
Korea, Republic of GSK Investigational Site Seoul
Korea, Republic of GSK Investigational Site Wonju
Netherlands GSK Investigational Site Almere
Netherlands GSK Investigational Site Amsterdam
Netherlands GSK Investigational Site Amsterdam
Netherlands GSK Investigational Site EDE
Netherlands GSK Investigational Site Heerlen
Netherlands GSK Investigational Site Rotterdam
New Zealand GSK Investigational Site Auckland
New Zealand GSK Investigational Site Dunedin
New Zealand GSK Investigational Site Hamilton
New Zealand GSK Investigational Site Lower Hutt
New Zealand GSK Investigational Site Otahuhu
New Zealand GSK Investigational Site Tauranga.
Norway GSK Investigational Site Ålesund
Norway GSK Investigational Site Bodø
Norway GSK Investigational Site Oslo
Norway GSK Investigational Site Tønsberg
Norway GSK Investigational Site Tromsø
Norway GSK Investigational Site Trondheim
Poland GSK Investigational Site Bydgoszcz
Poland GSK Investigational Site Bydgoszcz
Poland GSK Investigational Site Elblag
Poland GSK Investigational Site Lublin
Poland GSK Investigational Site Sopot
Poland GSK Investigational Site Torun
Poland GSK Investigational Site Wroclaw
Slovakia GSK Investigational Site Bratislava
Slovakia GSK Investigational Site Bratislava
Slovakia GSK Investigational Site Bratislava
Slovakia GSK Investigational Site Nitra
Slovakia GSK Investigational Site Nove Mesto nad Vahom
Slovakia GSK Investigational Site Presov
Slovakia GSK Investigational Site Trnava
South Africa GSK Investigational Site Bellville
South Africa GSK Investigational Site Claremont
South Africa GSK Investigational Site Observatory
South Africa GSK Investigational Site Parktown
Spain GSK Investigational Site Badalona
Spain GSK Investigational Site Elche
Spain GSK Investigational Site Galdakao/Vizcaya
Spain GSK Investigational Site Madrid
Spain GSK Investigational Site Sabadell (Barcelona)
Sweden GSK Investigational Site Göteborg
Sweden GSK Investigational Site Lund
Sweden GSK Investigational Site Stockholm
Sweden GSK Investigational Site Stockholm
Sweden GSK Investigational Site Umeå
United Kingdom GSK Investigational Site Birmingham
United Kingdom GSK Investigational Site Bristol
United Kingdom GSK Investigational Site Edinburgh
United Kingdom GSK Investigational Site Harrow Middlesex
United Kingdom GSK Investigational Site Manchester
United Kingdom GSK Investigational Site Newcastle-upon-Tyne
United Kingdom GSK Investigational Site Nottingham
United Kingdom GSK Investigational Site Oxford
United Kingdom GSK Investigational Site Salford
United States GSK Investigational Site Anaheim California
United States GSK Investigational Site Ann Arbor Michigan
United States GSK Investigational Site Atlanta Georgia
United States GSK Investigational Site Austin Texas
United States GSK Investigational Site Boston Massachusetts
United States GSK Investigational Site Chapel Hill North Carolina
United States GSK Investigational Site Chesterfield Michigan
United States GSK Investigational Site Chevy Chase Maryland
United States GSK Investigational Site Chicago Illinois
United States GSK Investigational Site Columbus Ohio
United States GSK Investigational Site Durham North Carolina
United States GSK Investigational Site Egg Harbor City New Jersey
United States GSK Investigational Site Germantown Tennessee
United States GSK Investigational Site Great Neck New York
United States GSK Investigational Site Hamden Connecticut
United States GSK Investigational Site Hammond Louisiana
United States GSK Investigational Site Houston Texas
United States GSK Investigational Site Indianapolis Indiana
United States GSK Investigational Site Jackson Mississippi
United States GSK Investigational Site Jacksonville Florida
United States GSK Investigational Site Jacksonville Florida
United States GSK Investigational Site Lakewood Colorado
United States GSK Investigational Site Lebanon New Hampshire
United States GSK Investigational Site Lee's Summit Missouri
United States GSK Investigational Site Lexington Kentucky
United States GSK Investigational Site Little Rock Arizona
United States GSK Investigational Site Littleton Colorado
United States GSK Investigational Site Los Angeles California
United States GSK Investigational Site Maitland Florida
United States GSK Investigational Site Monroe Louisiana
United States GSK Investigational Site Nashville Tennessee
United States GSK Investigational Site Oak Lawn Illinois
United States GSK Investigational Site Pasadena Texas
United States GSK Investigational Site Port Orange Florida
United States GSK Investigational Site Portland Oregon
United States GSK Investigational Site Raleigh North Carolina
United States GSK Investigational Site Rochester Minnesota
United States GSK Investigational Site San Antonio Texas
United States GSK Investigational Site San Diego California
United States GSK Investigational Site San Francisco California
United States GSK Investigational Site Seattle Washington
United States GSK Investigational Site Seattle Washington
United States GSK Investigational Site Towson Maryland
United States GSK Investigational Site Troy Michigan
United States GSK Investigational Site Tucson Arizona
United States GSK Investigational Site Tulsa Oklahoma
United States GSK Investigational Site Tupelo Mississippi
United States GSK Investigational Site Voorhees New Jersey

Sponsors (1)
Lead Sponsor Collaborator
GlaxoSmithKline

Countries where clinical trial is conducted

United States,  Australia,  Austria,  Belgium,  Canada,  Czechia,  Denmark,  France,  Germany,  Hungary,  Israel,  Italy,  Japan,  Korea, Republic of,  Netherlands,  New Zealand,  Norway,  Poland,  Slovakia,  South Africa,  Spain,  Sweden,  United Kingdom, 

Outcome
Type Measure Description Time frame Safety issue
Primary Percentage of Participants With Crohn's Disease Activity Index (CDAI) Response at Week 12 CDAI is a number which consists of information collected from a 7-day diary from the participants regarding symptoms. Remission is considered a score of 150 or less. Active disease is considered 200 or greater. A response to therapy is considered a decline in CDAI score of 70-points from baseline. The score was algorithmically derived from the sum of participant reported Crohn's disease symptoms recorded over 7 days and investigator recorded assessments of the participant's condition, laboratory parameters and use of anti-diarrhoeal medication. CDAI score was calculated based on the data collected in the diary card. The total CDAI score ranged from 0 to approximately 600, where higher scores indicate more severe disease. Both participants and investigators made their entries via IVRS each evening before going to bed. Percentage of participants with CDAI response at Week 12 was presented. Week 12
Secondary Percentage of Participants With CDAI Remission at Week 12 CDAI is a recognized scoring system to categorize disease severity with scores of >= 220 to <= 450 describing the moderately-to-severely active population. Clinical remission is defined as a CDAI score < 150 points if baseline CDAI is >= 150. If baseline CDAI is <150, the participant was not considered in remission. Participants with missing CDAI scores were considered not in remission according to the missing=no effect imputation. Percentage of participants in clinical remission at Week 12 was presented. Week 12
Secondary Percentage of Participants With a Clinical Response (CDAI Decrease From Baseline of >= 100 Points) at Both Week 8 and Week 12 Responders were defined as participants with CDAI decrease from baseline of >= 100 points. CDAI is a recognized scoring system to categorize disease severity with scores of >= 220 to <= 450 describing the moderately-to-severely active population. The score was algorithmically derived from the sum of participant reported Crohn's disease symptoms recorded over 7 days and investigator recorded assessments of the participant's condition, laboratory parameters and use of anti-diarrhoeal medication. Both participants and investigators made their entries via IVRS each evening before going to bed. Percentage of participants with CDAI decrease from baseline of >=100 points was presented. At Week 8 and 12
Secondary Percentage of Participants Achieving Clinical Remission (CDAI <150 Points) at Both Week 8 and Week 12 Clinical remission is defined as a CDAI score < 150 points if baseline CDAI is >= 150. If baseline CDAI is <150, the participant was not considered in remission. participants with missing CDAI scores were considered not in remission according to the missing=no effect imputation. Percentage of participants in clinical remission defined as a CDAI score of less than 150 points at other time points was presented. Week 8 and 12
Secondary Percentage of Participants With a Clinical Response (CDAI Decrease From Baseline of >=100 Points) at Week 8 CDAI is a recognized scoring system to categorize disease severity with scores of >= 220 to <= 450 describing the moderately-to-severely active population. The score was algorithmically derived from the sum of participant reported Crohn's disease symptoms recorded over 7 days and investigator recorded assessments of the participant's condition, laboratory parameters and use of anti-diarrhoeal medication. Both participants and investigators made their entries via IVRS each evening before going to bed. Percentage of Participants with a clinical response CDAI decrease from baseline of >=100 points at Week 8 was presented. Week 8
Secondary Percentage of Participant Achieving Clinical Remission (CDAI <150 Points) at Week 8 Clinical remission is defined as a CDAI score < 150 points if baseline CDAI is >= 150. If baseline CDAI is <150, the participant was not considered in remission. participants with missing CDAI scores were considered not in remission according to the missing=no effect imputation. Percentage of participants achieving clinical remission with CDAI <150 points at Week 8 was presented. Week 8
Secondary Change From Baseline in Inflammatory Bowel Disease Questionnaire (IBDQ) Total Score at Both Weeks 8 and 12 The IBDQ is a 32-item IBD-specific health related quality of life instrument evaluating general activities of daily living, intestinal function, social performance, personal interactions, and emotional status. Each item response was graded from 1 to 7 for each area evaluated. A higher score indicated better function in that area. Total IBDQ score was obtained by summing up scores for all 32 questions. Total IBDQ score ranged from 32 to 224. A higher score indicated better quality of life and lower score indicated worse quality of life. Day 1 assessment was considered as Baseline. Change from Baseline was calculated by subtracting value at Baseline from value at Weeks 8 and 12. Baseline (Week 0), Week 8 and Week 12
Secondary Incidence of Adverse Events (AE) and Serious Adverse Events (SAE) Data for number of participants who presented one or more adverse events (serious or non serious) was reported. An AE was defined as any untoward medical occurrence (MO) in a participant temporally associated with the use of a medicinal product (MP), whether or not considered related to the MP and can therefore be any unfavourable and unintended sign (including an abnormal laboratory finding), symptom, or disease temporally associated with its use. The SAE was any untoward MO that, at any dose, results in death, life threatening, persistent or significant disability/incapacity, results in or prolongs inpatient hospitalization, congenital abnormality or birth defect, that may not be immediately life-threatening or result in death or hospitalization but may jeopardize the participant or may require medical or surgical intervention to prevent one of the other outcomes listed in this definition. Up to Week 12
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