Paroxetine - Controlled Release in the Treatment of Irritable Bowel Syndrome (IBS)

Phase 4

Completed

• Conditions: Irritable Bowel Syndrome
• Interventions: Drug: Paroxetine CR; Drug: Placebo

• Registration Number: NCT00610909
• Lead Sponsor: Duke University

Brief Summary

Irritable bowel syndrome (IBS) is an extremely common disorder in the U.S population, affecting somewhere between 9-22% based on community based studies. IBS has a chronic relapsing course and overlaps with other functional gastrointestinal disorders. It accounts for high direct medical expenses and indirect costs including a significant degree of absenteeism. Most studies have suggested that there is a slight predominance among women, especially those that have suffered some form of physical or sexual trauma. It has been estimated that up to 25-40% of patients seen by gastroenterologists' are affected by IBS, and that 70-90% of these patients may have a psychiatric comorbidity, most commonly major depression and panic disorder, but also including schizophrenia, double depression, dysthymia and alcohol abuse.

Abdominal pain and disturbance of bowel habits characterize the symptoms of IBS in the absence of demonstrable structural pathology. The diagnosis of IBS relies upon clinical criteria alone, as there is no "gold standard" in laboratory findings. The diagnosis is dependent upon identifying characteristic symptoms, and then differentiating IBS from other structural bowel disorders. Previously, the diagnosis of IBS was based upon a consortium recommendation that examined and defined diagnostic criteria for over 100 functional gastrointestinal disorders. These criteria became the most definitive in the area of functional disorders and are referred to as the Rome Criteria. During the time since this consensus, these criteria have been modified, and in 1999 became the foundation for the second set of diagnostic criteria by consensus, now referred to as the Rome II criteria. The revised Rome II criteria include only the first part of the original criteria, but now require the presence of two out of three symptoms relating abdominal pain to bowel symptoms.

We designed our study and a Randomized, double-blind, parallel-group, flexible-dose, placebo-controlled 12-week study.

Detailed Description

Primary and Secondary Efficacy Measures Primary

Change from baseline in:

• Mean composite pain scores (on IVRS) Secondary

Change from baseline in:

* Associated symptoms of IBS (diarrhea, constipation, incomplete emptying, etc.) scores

* IBS Quality of Life scores

* Clinical Global Impression scores of 1 or 2

* Beck Depression Inventory II

* Beck Anxiety Inventory

Safety Measures

Safety and tolerability will be assessed through:

* Recording of spontaneous adverse events throughout the screening, run-in, and treatment phases of the study

* Conducting the DOTES at defined points during the study

All subjects withdrawn from the study will be followed until complete resolution of adverse events.

Study Schedule This is a placebo-controlled, double-blinded prospective 12-week study examining the efficacy of paroxetine extended release form in patients with IBS. Patients meeting the Rome II criteria for IBS will be recruited from the Duke University Medical Center Division of Gastroenterology and from the community. Patients found to satisfy these criteria will be referred for enrollment into this study. The study will be explained and informed consent obtained. A detailed history about the gastrointestinal symptoms and a physical exam will be performed. Laboratory evaluations (CBC, chemistry, fecal occult blood, urinalysis and EKG) will be obtained.

All patients will undergo a MINI at baseline to diagnose any comorbid Axis I psychiatric disorders, and a physical and sexual abuse history will be elicited. The patients will then have 1 week of symptom charting using the Interactive Voice Response System (IVRS) to measure baseline severity of IBS symptoms. Following that, patients will receive a single-blind placebo for a 1 week period. Those patients having a \>25% improvement in composite pain scores at the end of the placebo week or a CGI of 1 or 2 will be terminated from the study. Following the 1 week single-blind placebo lead-in, non-responders will be randomized to active drug or placebo for an additional period of 12 weeks. The patients will continue to fill out a daily symptom diary using the IVRS and, in addition, will have weekly visits (biweekly after week 4) to assess symptoms, side-effects, and improvement over the entire 12-week double-blind period. Those in the active treatment group will receive doses of Paxil CR in increments of 12.5 mg daily for the first week and increased at 12.5 mg increments at visit weeks to a maximum of 50 mg daily, as determined by the investigator. The investigator will adjust dosage based on clinical response. Following the completion of the double-blind phase, patients on placebo and non-responders to the study drug will be tapered off the study drug back to 0 over 2 weeks, and they will be referred to their Primary Care Physician, Internist or Gastroenterologist to be prescribed treatment for Irritable Bowel Syndrome. Patients on active drug (Paroxetine CR) who were successful responders during the double-blind phase will be eligible to continue on open label Paxil CR for an additional period of 6 months plus 2 weeks and will be followed on a monthly basis. They will complete the IVRS symptom diary for a week during each follow-up month for an additional 6 months. Those who completed the double-blind phase during the 1st half of the month (days 1-14) will complete the IVRS symptom diary for the first week beginning the 1st of the next month; those who completed the double-blind phase during the second half of the month (days 15-31) will complete the IVRS symptom diary for the first week beginning the 1st of the month following the next month. At the end of the 6-month period, study medication for these patients will be tapered back to 0 over 2 weeks, and they will be referred to their Primary Care Physician, Internist or Gastroenterologist to be prescribed treatment for the Irritable Bowel Syndrome. Placebo responders in the double-blind phase will not be eligible to enter the 6-month open label maintenance phase.

Clinical response will be measured in several ways. Abdominal pain severity will be measured with an ordinal scale rated from 1-9 (1=mild pain/discomfort, 9=very severe pain/discomfort). Abdominal pain frequency will be measured on a four-point scale (1=pain or discomfort present only occasionally, 2=pain or discomfort present less than half the day, 3= pain or discomfort present more than half the day, 4=pain or discomfort almost all day). The same ordinal scale will be used to quantify the distress or discomfort caused by feeling of incomplete evacuation, bloating or abdominal discomfort, and general level of stress or tension.

Sample Size Computation and Power Analysis Power considerations The calculations that follow are computed for the current design with an anticipated difference in pre-and post-treatment on the mean composite pain scores (on IVRS) of 25% (i.e. a reduction of score from 100 to 75). The means and standard deviations for this computation rely on our previous open-label studies of paroxetine and citalopram in IBS.

Assuming a strong effect size (0.5) of the primary variable (mean composite pain scores) and alpha set at 0.05, a projected sample size of 50 can detect the main effects with a power of greater than 0.95. If a lower effect size is assumed (0.4), a projected sample size of 55 can detect main effects with a power of approximately 0.94. Note that power may be reduced by attrition of the sample (i.e. dropouts) and also may be limited in testing secondary hypotheses where a further stratification of sample may be necessary (i.e. if the data is examined separately in men and women)

It may be more appropriate to have a sample size of 60 which allows for a 20% attrition rate and can still detect an effect size of 0.4 for the primary variable in the treatment-completer group with a power greater than 90.

Statistical analyses The study's main hypothesis is that paroxetine (Paxil CR) treatment will be more effective than placebo in reducing symptoms of IBS.

All statistical tests will be two sided at the 0.05 level of significance. Descriptive statistics will be used to provide a profile of demographic and outcome measures. Pearson product moment correlational analyses will be conducted to examine the relationships among variables. Baseline assessments between the two groups will be compared using chi square for categorical variables and independent t tests (two tailed) for continuous variables. Between group (medication/placebo) comparisons for primary and secondary variables will employ analysis of variance (ANOVA) with repeated measures. Assessments will be taken at baseline and end of week 1, 2, 3, 4, 6, 8, 10, and 12. Within group analyses (pre and end-of-treatment) will employ two tailed t tests.

To control for the possibility that current psychopathology might affect subject responding on interview and self-report instruments and otherwise modulate the treatment effects, the distribution of BDI-II and BAI scores and life time Axis I diagnoses in the placebo and control groups will be examined. The potential influence of any unequally distributed variables will be controlled via analyses-of covariance (ANCOVA) using the unequally distributed variables as covariates.

After the primary analysis other exploratory analyses will be conducted to test potential hypotheses for further studies.

Study Timeline

• Study Start: 2002-01
• Primary Completion: 2002-12
• Study Completion: 2002-12
• Status Verified: 2008-01
• Study First Submitted: 2008-01-28
• Study First Submitted QC: 2008-01-28
• Study First Posted: 2008-02-08
• Last Update Submitted: 2013-06-19
• Last Update Posted: 2013-06-20

Recruitment & Eligibility

• Status: COMPLETED
• Sex: All
• Target Recruitment: 60

Inclusion Criteria

Not provided

Exclusion Criteria

Not provided

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
1	Paroxetine CR	Those in the active treatment group will receive doses of Paxil CR in increments of 12.5 mg daily for the first week and increased at 12.5 mg increments at visit weeks to a maximum of 50 mg daily, as determined by the investigator. The investigator will adjust dosage based on clinical response. Following the completion of the double-blind phase, patients on placebo and non-responders to the study drug will be tapered off the study drug back to 0 over 2 weeks, and they will be referred to their Primary Care Physician, Internist or Gastroenterologist to be prescribed treatment for Irritable Bowel Syndrome.
2	Placebo	Same shape placebo

Primary Outcome Measures

Name	Time	Method
Change from baseline in: Changes in Mean composite pain scores (on IVRS)	12 weeks

Secondary Outcome Measures

Name	Time	Method
Change from baseline in Associated symptoms of IBS (diarrhea, constipation, incomplete emptying, etc.) scores IBS Quality of Life scores Clinical Global Impression scores of 1 or 2 Beck Depression Inventory II Beck Anxiety Inventory	12 weeks
Recording of spontaneous adverse events throughout the screening, run-in, and treatment phases of the study Conducting the DOTES at defined points during the study	12 weeks

Trial Locations

Locations (1)

Department of Psychiatry Clinical Trial Team, Duke University; 🇺🇸 Durham, North Carolina, United States