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NCT01903252 Clinical Trial

TP05 for the Treatment of Mild to Moderate Active Ulcerative Colitis (UC)

Acute Ulcerative Colitis Clinical Trial

Precision-UC

Official title:
A Randomised, Active-Controlled, Double-Blind and Open Label Extensions Study to Evaluate the Efficacy, Long-Term Safety and Tolerability of TP05 3.2g/Day for the Treatment of Active Ulcerative Colitis

Clinical Trial Details — Status: Completed

Administrative data
NCT number NCT01903252
Other study ID # TP0503
Secondary ID
Status Completed
Phase Phase 3
First received
Last updated
Start date July 2013
Est. completion date November 2016

Study information
Verified date August 2018
Source Tillotts Pharma AG
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

The purpose of this research study was to compare the medication TP05 to the medication Asacol™ for the treatment of ulcerative colitis (UC) and to assess the safety and tolerability of TP05. This study investigated whether TP05 is as good as (non-inferior to) Asacol™(1).

(1)The trademark Asacol™ is registered in over 55 countries as Asacol™ and as Octasa™, Fivasa™, Lixacol™, Asacolon™ in the United Kingdom, France, Spain and Ireland, respectively. The rights to Asacol, including the rights to the trademark, are owned by Tillotts Pharma AG in various countries except for the following: Switzerland, USA, United Kingdom, Canada, Italy, Belgium, the Netherlands and Luxembourg.

Description:

This is a Phase 3, randomised, double-blind, active-controlled, multi-centre, non-inferiority trial evaluating the safety and efficacy of 3.2 g of TP05/day compared to 3.2 g/day of Asacol™ with an open label extension to assess the long-term safety and tolerability of TP05 administered over a 26 week period. A total of 817 subjects with mildly to moderately active UC were evaluated. Eligible subjects were randomly assigned in a 1:1 ratio to receive 3.2 g/day of TP05 (administered once daily(OD)) or 3.2 g/day of Asacol™. The primary efficacy outcome was assessed at Week 8. All subjects who respond to TP05/Asacol™ (response or remission) continued receiving blinded study treatment for up to 12 weeks. After that, subjects could enroll in an Open Label Extension (OLE) for 26 weeks duration to receive TP05. Subjects failing to respond to study drug at the Week 8 visit could enroll in the OLE at week 8 and received 4.8 g/day of TP05.

Recruitment information / eligibility
Status Completed
Enrollment 817
Est. completion date November 2016
Est. primary completion date May 2016
Accepts healthy volunteers No
Gender All
Age group 18 Years and older
Eligibility Induction phase - Main criteria for inclusion include:

1. Male or non-pregnant, non-lactating females, 18 years of age or older. Females of child bearing potential must have a negative serum pregnancy test prior to randomisation, and must use a hormonal (oral, implantable or injectable) or barrier method of birth control throughout the study. Females unable to bear children must have documentation of such in the source records (i.e., tubal ligation, hysterectomy, or post-menopausal [defined as a minimum of one year since the last menstrual period]).

2. Documented diagnosis of UC with disease extending at least 15 cm from the anal verge.

3. Active UC defined by:

- a. Mayo score of = 5

- b. Sigmoidoscopy component score = 2 confirmed by central review and

- c. Rectal bleeding component score = 1

4. Ability of the subject to participate fully in all aspects of this clinical trial.

5. Written informed consent must be obtained and documented.

Induction Phase - Main criteria for exclusion include:

Subjects who exhibit any of the following conditions are to be excluded from the study:

(1) Severe UC defined by the following criteria: 6 bloody stools daily with one or more of the following:

- a. oral temperature > 37.8 degrees C or > 100.0 degrees F

- b. pulse > 90 beats/min

- c. haemoglobin < 10 g/dL (2) Treatment with oral mesalamine at a dose of > 2.4 g/day within 4 weeks prior to randomisation.

(3) Treatment with topical therapy (mesalamine or corticosteroids) within 2 weeks prior to randomisation (4) Treatment with systemic or rectal steroids within 4 weeks prior to randomisation.

(5) Treatment with immunosuppressants within 6 weeks prior to randomisation. (6) Treatment with infliximab or other biologics within 3 months prior to randomisation.

(7) Treatment with antibiotics within 7 days prior to randomisation. (8) Treatment with probiotics within 7 days prior to randomisation. (9) Treatment with anti-diarrhoeal treatment within 7 days prior to randomisation.

(10) Treatment with nicotine patch within 7 days prior to randomisation. (11) Received any investigational drug within 30 days prior to randomisation. (12) History of colectomy or partial colectomy. (13) History of definite dysplasia in colonic biopsies. (14) Crohn's disease. (15) Immediate or significant risk of toxic megacolon. (16) Known bleeding disorders. (17) Hypersensitivity to salicylates, aspirin, sulfasalazine or mesalazine. (18) Serum creatinine > 1.5 times the upper limit of the normal range. (19) Aspartate aminotransferase (AST), alanine aminotransferase (ALT), total bilirubin or alkaline phosphatase > 2 times the upper limit of the normal range.

(20) Serious underlying disease other than UC which in the opinion of the investigator may interfere with the subject's ability to fully participate in the study.

(21) History of alcohol or drug abuse which in the opinion of the investigator may interfere with the subject's ability to comply with the study procedures.

(22) Stools positive for Clostridium difficile toxin. (23) Pregnant or lactating women. (24) Prior enrolment in the study.

OLE - Main criteria for inclusion include:

1. Attendance at the Week 8 visit and completion of disease activity assessments prior to enrolment in OLE at Week 12 (responders or remitters) or Week 8 (non-responders).

2. At least 75% compliance with study medication in the induction phase.

OLE - Main criteria for exclusion include:

(1) Withdrawal from the induction phase prior to the Week 8 visit.

Study Design

Related Conditions & MeSH terms

Intervention

Drug:
TP05
3.2g/day once daily for 12 weeks (blinded), 1.6g/d - 4.8g/d up to week 38 (open label)
Asacol 400 mg
3.2g/d twice daily for 12 weeks (blinded), switch to 1.6g/ - 4.8g/d TP05 up to week 38 (open label)

Locations
Country Name City State
Switzerland Tillotts Pharma AG Rheinfelden Baslerstrasse 15

Sponsors (1)
Lead Sponsor Collaborator
Tillotts Pharma AG

Country where clinical trial is conducted

Switzerland, 

Outcome
Type Measure Description Time frame Safety issue
Primary Period 1: Clinical and Endoscopic Remission Mayo Score of <= 2 points with no individual sub-score > 1 Week 8
Primary Period 2: Clinical Response, Open-Label Extended Induction A decrease in the PMCS of = 2 points and = 30% from baseline, with a decrease in the rectal bleeding sub-score of = 1 point or absolute rectal bleeding sub-score of 1 or 0. Week 16
Primary Period 3: Clinical Remission Clinical Remission was defined as a score of 0 points for both stool frequency and rectal bleeding on the Partial Mayo Clinic Score (PMCS) Week 38
Secondary Period 1: Endoscopic Remission Endoscopic remission was defined as a Mayo endoscopy subscore of 0 Week 8
Secondary Period 1: Endoscopic Response Endoscopic response was define as a reduction in the Mayo endoscopic sub score of at least one. Week 8
Secondary Period 1: Clinical Remission Clinical Remission was defined as a score of 0 points for both stool frequency and rectal bleeding on the Partial Mayo Clinic Score (PMCS) Week 8
Secondary Period 1: Rectal Bleeding Sub-score of 0 Rectal bleeding sub-score of 0 was defined as a sub score on the rectal bleeding component of the Mayo score Week 8
Secondary Period 1: Clinical and Endoscopic Response Clinical and Endoscopic Response was defined as a decrease in the Mayo score of =3 points from baseline and a reduction of = 30% from baseline with either an accompanying decrease in the rectal bleeding sub-score of at least 1 point or an absolute rectal bleeding sub-score of 0 or 1 at the Week 8 visit. If a subject withdrew from the study prior to Week 8 or their response status was not evaluable due to incomplete and/or invalid data, the subject was considered a non-responder. Week 8
Secondary Period 1: Clinical Remission Clinical Remission was defined as a score of 0 points for both stool frequency and rectal bleeding on the Partial Mayo Clinic Score (PMCS) Week 12
Secondary Period 1: Clinical Response A decrease in the PMCS of = 2 points and = 30% from baseline, with a decrease in the rectal bleeding sub-score of = 1 point or absolute rectal bleeding sub-score of 1 or 0. Week 12
Secondary Period 1: Rectal Bleeding Score of 0 Rectal bleeding sub-score of 0 was defined as a sub score on the rectal bleeding component of the Mayo score Week 12
Secondary Period 1: Clinical Remission at Both Week 8 and 12 Clinical Remission was defined as a score of 0 points for both stool frequency and rectal bleeding on the Partial Mayo Clinic Score (PMCS) Week 8 and week 12
Secondary Period 1: Clinical Response at Both Week 8 and Week 12 A decrease in the Partial Mayo Score of = 2 points and = 30% from baseline, with a decrease in the rectal bleeding sub-score of = 1 point or absolute rectal bleeding sub-score of 1 or 0. Week 8 and Week 12
Secondary Period 1: Change in Mayo Score From Baseline Between-Group Difference of Mayo Score, Change from Baseline The changes from baseline to week 8 values in Mayo scores are compared between the two treatment groups.
The Mayo scoring system is a well-established tool for assessing UC disease activity. The Mayo score is the sum of 4 component sub-scores, each scored on a scale ranging from 0 representing no pathology to 3 for severe disease. The 4 component sub-scores consist of, 1) stool frequency, 2) rectal bleeding, 3) flexible sigmoidoscopy scores, and 4) physician's global assessment. A Mayo score of 0 indicates no pathology and a score of 12, severe disease. Change from Baseline is calculated Baseline-score minus week 8-score. A larger change in Mayo score from baseline when patients experienced acute disease, indicates improvement and treatment success.		 Baseline and Week 8
Secondary Period 1: Change in Partial Mayo Score From Baseline Between-Group Difference of Partial Mayo Score, Change from Baseline to Week 8 The Partial Mayo Score is the sum of the component sub-scores, 1) stool frequency, 2) rectal bleeding and 3) physician's global assessment. A partial Mayo Score of 0 indicates no disease and a maximum score of 9 indicates severe symptoms. Change from Baseline is calculated Baseline-score minus week 8-score. A larger change in Partial Mayo Score from Baseline where patients experienced acute disease, indicates improvement and treatment success. Baseline and Week 8
Secondary Period 1: Change in Stool Frequency Score Between-Group Difference of Stool Frequency Score, Change from Baseline The changes from baseline to week 8 values in stool frequency will be compared between the two treatment groups. Values for stool frequency range between 0 and 3. A value of 0 indicates normal stool frequency, a value of 3 indicates 5 or more stools than normal. Change from Baseline is calculated Baseline-score minus week 8-score. A large difference between week 8 values and baselines indicates treatment success. Baseline and Week 8
Secondary Period 1: Change in Rectal Bleeding Score From Baseline Between-Group Difference of Rectal Bleeding Score, Change from Baseline The changes from baseline to week 8 values in rectal bleeding scores will be compared between the two treatment groups. A value of 0 indicates no rectal bleeding, a value of 3 indicates only blood is passing. Change from Baseline is calculated Baseline-score minus week 8-score. A large difference at week 8 compared to baseline is indicative of treatment success. Baseline and Week 8
Secondary Period 1: Change in Physician Global Assessment Score From Baseline Between-Group Difference of Physician Global Assessment Score, Change from Baseline.
The changes from baseline to week 8 values in the Physician Global Assessment score will be compared between the two treatment groups. A value of 0 means no pathology and a value of 3 means severe disease. Change from Baseline is calculated Baseline-score minus week 8-score. A large difference between baseline to week 8 indicates treatment success.		 Baseline and Week 8
Secondary Period 1: Change in Endoscopic Score From Baseline Between-Group Difference of Endoscopic Score, Change from Baseline. The changes from baseline to week 8 values in sigmoidoscopic (mucosal) appearance scores will be compared between the two treatment groups. A value of 0 in the endoscopic score means normal or inactive disease and a value of 3 means severe disease. Change from Baseline is calculated Baseline-score minus week 8-score. A large difference between baseline to week 8 indicates treatment success. Baseline and Week 8
Secondary Period 2: Clinical Remission Clinical Remission was defined as a score of 0 points for both stool frequency and rectal bleeding on the Partial Mayo Clinic Score (PMCS) Week 16
Secondary Period 2: Rectal Bleeding Sub-score of 0 Percentage of patients achieving the endpoint rectal bleeding sub-score of 0 Week 16
Secondary Period 2: Stool Frequency 0 Percentage of patients achieving the endpoint stool frequency sub-score of 0 Week 16
Secondary Period 2: Urgency Percentage of patients achieving an Urgency Score of 0. A score of 0 indicates no urgency reported in any of the three days prior to the visit at week 16. A score of 1 indicates urgency reported in any of the three days prior to the visits. Week 16
Secondary Period 2: UC-Related Complications Percentage of Patients Experiencing Complications related to UC Week 16
Secondary Period 3: Clinical Response A decrease in the PMCS of = 2 points and = 30% from baseline, with a decrease in the rectal bleeding sub-score of = 1 point or absolute rectal bleeding sub-score of 1 or 0. Week 38
Secondary Period 3: Clinical and Endoscopic Remission Mayo Score of <= 2 points with no individual sub-score > 1 Week 38
Secondary Period 3: Clinical and Endoscopic Response Both has to be achieved, Clinical and Endoscopic Response which is defined by a decrease from baseline in the Mayo score of = 3 points and > 30% of the baseline score, with an accompanying decrease in the rectal bleeding sub-score of = 1 point or an absolute rectal bleeding sub-score of 0 or 1. Week 38
Secondary Period 3: Endoscopic Remission Percentage of each dose group achieving an endoscopy sub score of 0 Week 38
Secondary Period 3: Endoscopic Response Endoscopic response was define as a reduction in the Mayo endoscopic sub score of at least one. Week 38
Secondary Period 3: Rectal Bleeding Sub Score of 0 Percentage of each dose group achieving the endpoint rectal bleeding subscore 0 Week 38
Secondary Period 3: Stool Frequency Sub-score 0 Patients achieving a Stool Frequency sub-score of 0 Week 38
Secondary Period 3: No Urgency No urgency is a score of 0 and indicates that patients did not report urgency during any of the three days prior to the visit at week 38. A score of 1 indicates that urgency was reported during any of these three days. Week 38
Secondary Period 3: UC-Related Complications Percentage of Patients with Complications related to UC Week 38