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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT02757105
Other study ID # RHB-102-02
Secondary ID
Status Completed
Phase Phase 2
First received
Last updated
Start date May 19, 2016
Est. completion date July 14, 2017

Study information

Verified date July 2018
Source RedHill Biopharma Limited
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

This is a randomized, double-blind, placebo-controlled, 2-arm parallel group study. After qualifying for the study and signing informed consent, patients will undergo a two-week observation period during which stool consistency and frequency data and symptom data will be collected. Patients will then be randomized 60:40 to RHB-102 12 mg (BEKINDA) or placebo. Patients will continue on treatment for 8 weeks. Each medication will be given once daily.


Description:

All patients will undergo baseline evaluation including full history and physical, with particular attention to gastrointestinal symptomatology and findings, a standard set of safety laboratory examinations (CBC and platelet count, biochemical profile, urinalysis, serum thyroid-stimulating hormone (TSH) and free T4, INR), and 12-lead ECG. In addition, the following studies will be performed to exclude other causes of gastrointestinal symptoms:

- Serum testing for C-reactive protein and gluten sensitivity

- Colonoscopy if required per protocol

- Patients with a history of positive tests for ova, parasites or Clostridium difficile must undergo repeat testing, which must be negative, during the screening period. Starting during the baseline observation phase, all patients will keep diaries of symptomatology and stool frequency and consistency. Stool consistency will be assessed according to the Bristol Stool Form scale (Lewis and Heaton, 1997).

Patients will keep diaries of stool frequency and consistency, symptoms, study medication compliance, and use of all medications, including rescue medications, throughout the study.

Serum electrolyte assays (bicarbonate, calcium, chloride, magnesium, potassium, and sodium) will be performed at week 3 on study. Safety laboratory examinations will be performed during and after the treatment period in accordance with the study procedures schedule below.

Patients will be questioned periodically regarding concomitant medication use and the occurrence of adverse events.

Patients must complete at least 12 days of all baseline diary entries within the 14 day screening period to be eligible to participate in the study. Patients completing fewer than 12 days of diary entries may, at the investigator's discretion, repeat the screening period diary. As long as the patent can complete and enter the study within 6 weeks, baseline laboratory studies need not be repeated. If repeating the 2 weeks' baseline diary will result in a period longer than 6 weeks from consent to start of treatment, the medical monitor must be consulted prior to randomization.


Recruitment information / eligibility

Status Completed
Enrollment 127
Est. completion date July 14, 2017
Est. primary completion date June 16, 2017
Accepts healthy volunteers No
Gender All
Age group 18 Years to 80 Years
Eligibility Inclusion Criteria:

1. Male and female patients age=18 years (with a minimum of 35% males in the study)

2. Patient meets FDA guidance and Rome III criteria for IBS-D:

a. Recurrent abdominal pain or discomfort over =6 months, with frequency =3 days/month in the last 3 months associated with =2 of the following: i. Improvement with defecation ii. Onset associated with a change in frequency of stool iii. Onset associated with a change in the form of stool b. Loose or watery stools (Bristol stool form scale 6 or 7) =2 days per week

3. Average worst daily pain intensity =3.0 for each of the two baseline weeks

4. Major laboratory parameters within the following limits (no worse than grade 1 abnormalities per NCI-CTCAE v4):

a. Adequate hematologic function, as demonstrated by i. Hemoglobin =10 g/dL ii. Absolute neutrophil count (ANC) 1.5-10 x 10^9/L iii. Platelets =100 x 10^9/L b. Adequate liver and renal function as demonstrated by i. Aspartate transaminase (AST) and Alanine transaminase (ALT) each = 3.0 x upper limit of normal (ULN) ii. Total bilirubin =1.5 x ULN iii. Creatinine =1.5 X ULN c. Euthyroid based on thyroid-stimulating hormone (TSH) and free T4 levels

5. Patients on thyroid hormone replacement must be on a stable dose for at least one month prior to study entry.

6. C-reactive protein =2 x ULN for lab

7. Patients of childbearing potential and male patients with partners of childbearing potential must utilize effective contraceptive measures Women of childbearing potential are women who have menstruated in the past 12 months, with the exception of women who have undergone surgical sterilization

8. All patients must sign informed consent.

Exclusion Criteria:

1. Evidence of other cause for bowel disease:

1. Relevant abnormalities seen on colonoscopy if previously performed or if required per this protocol. These include but are not limited to Crohn's disease, ulcerative colitis, diverticulitis, ischemic colitis, microscopic colitis.

2. History of and/or positive serologic test for celiac disease

3. Known or suspected lactose intolerance.

2. History of abdominal surgery other than appendectomy or cholecystectomy at any time

3. Any elective major surgery (of any organ) planned for the period of the study, including follow-up

4. History of organic abnormalities of the GI tract including but not limited to intestinal obstruction, stricture, toxic megacolon, GI perforation, fecal impaction, gastric banding, adhesions or impaired intestinal circulation (e.g., aortoiliac disease)

5. Current or previous diagnosis of neoplasia (except non-GI neoplasia in complete remission =5 years, squamous and basal cell carcinomas). With approval of the medical monitor patients with curatively treated neoplasm in complete remission <5 years may be entered in the study.

6. Patients with a history of positive tests for ova or parasites or Clostridium difficile must be retested during the screening period and tests for the relevant agents must be negative

7. Use of any 5-HT3 antagonist (5hydroxytryptamine receptor antagonists) within 4 weeks of the start of baseline data collection.

8. Use of rifaximin within 4 months of the start of baseline data collection.

9. Use of any other agent specific for IBS (such as alosetron or eluxadoline) or for symptomatic treatment of IBS (such as antispasmotics and antidiarrheals other than loperamide) within 2 weeks of the start of baseline data collection.

10. Uses of any investigational agent for any indication within 4 weeks of the start of baseline data collection.

11. Congestive heart failure, bradyarrhythmia (baseline pulse<55/min), known long QT syndrome

12. Patients who have Corrected QT interval (QTc) prolongation>450 msec noted on screening ECG, or who are taking medication known to cause QT prolongation

Note: For current list of medications known to cause QT prolongation see:

https://www.crediblemeds.org/healthcare-providers/drug-list/ There are several risk categories. Use the list showing those drugs known to cause torsade de pointes (TdP)

13. Hypersensitivity or other known intolerance to ondansetron or other 5-HT3 antagonists

14. Patient has taken apomorphine within 24 hours of screening

15. Pregnant or lactating

16. Patients with other major illnesses, either physical or psychiatric, or social situations which may interfere with participation in the study or interpretation of results

17. Patients with severe hepatic impairment, defined as Child-Pugh score =10 at baseline

Study Design


Related Conditions & MeSH terms


Intervention

Drug:
BEKINDA

Placebo


Locations

Country Name City State
United States Bristol Hospital Dba Connecticut Gastroenterology Institute Bristol Connecticut
United States Aztec Medical Research, LLC Channelview Texas
United States Clinsearch Chattanooga Tennessee
United States Prx Clinical Garden Grove California
United States Clinical Research of Homestead Homestead Florida
United States Clinical Research Associates, LLC Huntsville Alabama
United States E Squared Research, Inc. Huntsville Alabama
United States New Phase Research & Development Knoxville Tennessee
United States Endoscoopy Center of AR Little Rock Arkansas
United States Great Lakes Medical Research Mentor Ohio
United States Providence Clinical Research North Hollywood California
United States Arkansas Gastroenterology, P.A. North Little Rock Arkansas
United States Gastroenterology Research of San Antonio San Antonio Texas
United States Shahram Jacobs MD, Inc. Sherman Oaks California
United States Advanced Rx Clinical Research Group, Inc. Westminster California
United States PMG Research of Winston-Salem Winston-Salem North Carolina

Sponsors (1)

Lead Sponsor Collaborator
RedHill Biopharma Limited

Country where clinical trial is conducted

United States, 

Outcome

Type Measure Description Time frame Safety issue
Primary Summary and Analysis of Overall Stool Consistency Response Rate - mITT Population A weekly stool consistency responder was defined in the FDA guidance on IBS-D as a patient who experienced (during a week) a =50% reduction in the number of days with at least one stool that has a consistency of Type 6 or 7 on the Bristol stool scale compared with baseline. In addition, to be considered a responder for the week, the patient could not have had an increase in average abdominal pain >10% over baseline during that week. A patient was characterized as an overall stool consistency responder if the patient was a weekly responder for at least 50% of the planned weeks of treatment. 8 weeks
Primary Summary and Analysis of Overall Stool Consistency Response Rate Males - mITT Population A weekly stool consistency responder was defined in the FDA guidance on IBS-D as a patient who experienced (during a week) a =50% reduction in the number of days with at least one stool that has a consistency of Type 6 or 7 on the Bristol stool scale compared with baseline. In addition, to be considered a responder for the week, the patient could not have had an increase in average abdominal pain >10% over baseline during that week. A patient was characterized as an overall stool consistency responder if the patient was a weekly responder for at least 50% of the planned weeks of treatment. 8 weeks
Primary Summary and Analysis of Overall Stool Consistency Response Rate Females - mITT Population A weekly stool consistency responder was defined in the FDA guidance on IBS-D as a patient who experienced (during a week) a =50% reduction in the number of days with at least one stool that has a consistency of Type 6 or 7 on the Bristol stool scale compared with baseline. In addition, to be considered a responder for the week, the patient could not have had an increase in average abdominal pain >10% over baseline during that week. A patient was characterized as an overall stool consistency responder if the patient was a weekly responder for at least 50% of the planned weeks of treatment. 8 weeks
Primary Summary and Analysis of Overall Stool Consistency Response Rate: Sensitivity Analysis Without Imputation for Use of Rescue Medication - mITT Population A weekly stool consistency responder was defined in the FDA guidance on IBS-D as a patient who experienced (during a week) a =50% reduction in the number of days with at least one stool that has a consistency of Type 6 or 7 on the Bristol stool scale compared with baseline. In addition, to be considered a responder for the week, the patient could not have had an increase in average abdominal pain >10% over baseline during that week. A patient was characterized as an overall stool consistency responder if the patient was a weekly responder for at least 50% of the planned weeks of treatment. 8 weeks
Primary Summary and Analysis of Overall Stool Consistency Response Rate by Baseline CRP > Median - mITT Population A weekly stool consistency responder was defined in the FDA guidance on IBS-D as a patient who experienced (during a week) a =50% reduction in the number of days with at least one stool that has a consistency of Type 6 or 7 on the Bristol stool scale compared with baseline. In addition, to be considered a responder for the week, the patient could not have had an increase in average abdominal pain >10% over baseline during that week. A patient was characterized as an overall stool consistency responder if the patient was a weekly responder for at least 50% of the planned weeks of treatment. 8 weeks
Primary Summary and Analysis of Overall Stool Consistency Response Rate by Baseline CRP = Median - mITT Population A weekly stool consistency responder was defined in the FDA guidance on IBS-D as a patient who experienced (during a week) a =50% reduction in the number of days with at least one stool that has a consistency of Type 6 or 7 on the Bristol stool scale compared with baseline. In addition, to be considered a responder for the week, the patient could not have had an increase in average abdominal pain >10% over baseline during that week. A patient was characterized as an overall stool consistency responder if the patient was a weekly responder for at least 50% of the planned weeks of treatment. 8 weeks
Secondary Summary and Analysis of Overall Worst Abdominal Pain Response Rate - mITT Population A weekly pain responder was defined as a patient who experienced a decrease in the weekly average of worst abdominal pain in the past 24 hours score =30% compared with baseline and no increase in the number of days per week with Type 6 or 7 stool consistency. An overall pain responder was defined as a patient who was a weekly pain responder for at least 50% of the planned weeks of treatment. 8 weeks
Secondary Summary and Analysis of Overall Study Response Rate - mITT Population A patient was characterized as an overall weekly responder if the patient met both the stool consistency and pain response definitions for a given week. A patient was characterized as a composite study responder if the patient met the criteria for both weekly stool consistency and pain response for at least 50% of the planned weeks of treatment. 8 weeks
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