Irritable Bowel Syndrome Clinical Trial
Official title:
Efficacy and Safety of Chinese Medicine JCM-16021 for Diarrhea-predominant Irritable Bowel Syndrome: a Multicenter, Randomized, Double-blind, Placebo Controlled Clinical Trial
This is a multicenter, randomized, double-blind, placebo controlled clinical trial, in order to evaluate the efficacy and safety of Chinese Medicine JCM-16021 for diarrhea-predominant irritable bowel syndrome. All patients will be evaluated for study eligibility at Visits 1 (baseline) and 2 (2 weeks). On visit 2, patients who meet the criteria will be randomly assigned to receive 8-week treatment of either JCM-16021 Granules or JCM-16021 placebo Granules. The investigators, research assistants and participants are not aware of the treatment assignments throughout the study. Treatment codes will only be broken after the completion of study. The assessments at Visit 3 (4-week post treatment) and at visit 4 (end of 8-week treatment) are used to measure treatment response (i.e. changes from baseline). Assessment at visit 5 (end of 8-week follow up) is to determine any sustained response to treatment. All the visits will be carried out in HKBU and CUHK clinics.
Sample size calculation:
Sample size is calculated on the basis of primary efficacy variables. From our previous
study, the global assessment of improvement (GAI) were 52% in herbal medicine group and 32%
in western medicine group, respectively. According to the references (Corazziari E, Bytzer P,
Delvaux M, et al. Clinical trial guidelines for pharmacological treatment of irritable bowel
syndrome. Alimentary pharmacology & therapeutics 2003; 18 (6): 569-580), the investigational
drug is more effective than placebo (the overall improvement rate of symptoms is 15%), using
StudySize2.0 software to calculate the sample size, assuming the improvement in the treatment
group is 52%. In order to detect a difference with a two-side p value <0.05 and 80%
statistical power, we will need to recruit 166 patients per arm. Further assuming a 15%
dropout rate, we conclude that a total of 392 patients (196 per arm) will be recruited to
ensure statistically significant results.For the number of cases distribution between
centers, according to the references (Lai D,Chang KC, Rahbar MH, Moye LA. Optimal Allocation
of Sample Sizes to Multicenter Clinical Trials. Journal of biopharmaceutical statistics 2013;
23 (4): 818-828) , from the following equation, we will consider the center about the patient
flow, traffic, treatment,costs and other possible factors, we will use the formula below to
estimate the number of cases that will be recruited in each center.
Research medical record and Electronic Database:
All patients should be observed and assessed based on clinical trial protocol and the
investigators need to document in the medical record accurately and clearly. Research medical
record is the source document which cannot be altered. Any correction should not change the
original record and can only be added in a way of narration with reasons. The doctor
participated in the clinical trial needs to sign and date the record. An electronic database
will be created. Each study site will input their own data and be responsible for its
accuracy. A chief statistician will be responsible for data cleaning and data analysis.
Analysis parameters:
All parameters and study elements will be analyzed. The statistical analysis will be
performed using SAS 9.1 and SPSS software.
Analysis sets:
Full analysis set (FAS): The analysis will be conducted according to the intention-to-treat
(ITT) principle which means to eliminate the participants with a minimum and reasonable
method. ITT population refers to all participants who go through randomization, enter
double-blind treatment period, and receive IMP at least one time. Missing values of efficacy
will be imputed by the last-observation-carried forward (LOCF) method. Per-protocol set (PP):
PP population refers to all participants who complete relative observation according to
protocol requirement and are confirmed to meet following conditions: ① compliance between 80%
and 120%; ② not taking probihited medications during the process of trial; ③ meeting
inclusion criteria and not fitting any exclusion items; ④ completing all planned visits and
necessary items of CRF. Missing values of this set will still be processed as missing data
and not be imputed. Safety analysis set: Population for safety analysis refers to all
participants who enter the trial, receive medication at least one time and have suitable
follow-up data for safety analysis. All safety data including AEs and laboratory results from
participants will be assessed.16.3 Statistical analysis technique Baseline data (gender, age,
race, weight, height, vital signs, course of IBS, history of smoking and alcohol) will be
descriptively summarized. Differences of measurement data between the groups will be assessed
with the use of t-test for normally distributed continuous variables and Wilcoxon signed rank
test for non-normally distributed. Differences of enumeration data between the groups will be
assessed with the use of chi-square test or CMH test when considering multicenter character.
Measurement data of different groups in each visit will be reported as mean ± standard
deviation (SD). Intra-group comparisons between baseline and each visit will be conducted by
using paired t-test (or Wilcoxon signed rank test). Comparisons between groups will be
conducted by using an analysis of variance (ANOVA), with other confounding factors like
multicenter character conducting the covariate analysis. Statistical analysis for the data
which do not meet above conditions (e.g. non-normal) will be conducted with the use of
non-parametric test. Enumeration data of different groups in each visit will be reported as
frequency (proportion). Comparisons between groups will be assessed with the use of X2 test
(CMH test) or non-parametric test. Dropout analysis: Dropout analysis will be conducted with
the use of chi-square test. If the data do not conform to chi-square test (data include 0, or
theoretical frequency is below 1), Fisher's exact test will be used. Compliance analysis:
Compliance analysis will be conducted with the use of chi-square test. If the data do not
conform to chi-square test (data include 0, or theoretical frequency is below 1), Fisher's
exact test will be used.
Hypothesis testing:
This trial will conduct superiority analysis firstly. Other difference test will be conduct
by two-sided test. The statistical significance will be defined as two-sided P-value of ≤0.05
without any special explanation.
Efficacy analysis:
The efficacy analysis will be conducted with the use of PP analysis and ITT analysis in the
meantime. Comparisons of measurement data will be conducted by using analysis of covariance
(ANCOVA), with treatment group and trial center as a factor in the model and baseline as the
covariate. Comparisons of measurement data will be conducted by using chi-square test or CMH
chi-square test when considering multicenter character. Meanwhile, superiority analysis
between experimental group and control group will be conducted based on primary efficacy
variables. Superiority test depends on interval method.
Safety analysis:
Extent of exposure: Descriptive statistics will be conducted according to the exposure dose
and time of medication in different groups. AEs analysis: Comparisons of incidence rate of
AEs between groups will be conducted with the use of X2 test. And investigators need to list
and describe the AEs happened in this trial. If the data do not conform to X2 test (data
include 0, or theoretical frequency is below 5), Fisher's exact test will be used.
Data management:
CRFs are filled in by investigators and study coordinators, other assessment forms by every
participant (including dropout cases). Data processing will be conducted in accordance with
the following protocol:
1. Verification of CRFs: Study coordinators need to verify CRFs before inputting.
2. Data verification needs to be conducted successively in the following two steps:
1. Verify the consistency and logicality of data: Review contents of data range and
logicality are determined by the range of each indexes and the interrelation.
Corresponding software will also be written to correct the incorrect data.
2. Compare database and CRFs by manual testing. Selectively counter check 10% CRFs
with participants' medical notes to know the quality of inputting and analyze and
handle the existing problems.
3. Data inspection and closure of database: After verifying the validity of established
database and statistical protocol, principal investigators, will lock the data. The
locked data are not allowed to change. Confirmed problems found after locking will be
handled in the process of statistical analysis. All mistakes and modification should be
recorded and kept properly.
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