Clinical Trial Details
— Status: Terminated
Administrative data
| NCT number |
NCT02053350 |
| Other study ID # |
17576 |
| Secondary ID |
17576 Protocol_A |
| Status |
Terminated |
| Phase |
Phase 2
|
| First received |
|
| Last updated |
|
| Start date |
April 2015 |
| Est. completion date |
April 5, 2017 |
Study information
| Verified date |
May 2022 |
| Source |
University of Virginia |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
The aim of this study is to test the efficacy of alanyl-glutamine supplementation in the
treatment of C. difficile infection. We hypothesize that alanyl-glutamine when given with
standard antibiotic treatment for C. difficile infection will decrease diarrhea, mortality
and recurrent disease.
Description:
This is a Phase II randomized, placebo-controlled, double-blinded, dose-ranging study to
determine optimal effective dose and safety of AQ between 0, 4, 24, and 44 g doses
administered orally for ten days concurrent with standard treatment (oral vancomycin at UVa)
among first time incident cases of uncomplicated CDI in hospitalized persons age 50 and
older. Our hypothesis is that AQ will reduce recurrence (primary outcome) and mortality
(secondary outcome) at 60 days post-treatment. Furthermore, we hypothesize that
alanyl-glutamine supplementation will be associated with decreased intestinal and systemic
inflammation and improvement of intestinal microbial and metabolic profiles. We plan to
enroll 260 patients, equally divided into 4 arms. Upon enrollment, participants will be
randomized to either receive AQ at 4, 24, or 44 g or placebo (water). Study agent is
administered once a day, orally or enterally, if feeding tube is present. Because we are
enrolling subjects over a longer period of time, we will utilize block randomization to
ensure that relative temporal balance is maintained throughout the trial. Participants will
be followed up daily during treatment for adverse event monitoring and weekly for 60 days
post-treatment for recurrences and survival. Blood, urine and stool specimens will be
collected at days 0, 10 and 70 to assay for markers of inflammation and microbial and
metabolic profiling.
The data set utilized for all initial baseline feature and demographic reporting will be the
Intention to Treat Analysis Dataset, which will be comprised of all randomized participants.
The primary dataset will be a Modified Intention to Treat Analysis Dataset for all endpoints,
comprised of all participants who took at least one dose of study intervention (placebo or
treatment), regardless of completeness of follow-up outcome data. The Safety Analysis Dataset
will be all participants who took at least one dose of study intervention. The Per Protocol
Analysis Dataset will be those patients who took at least 9 doses of study intervention for 9
days of the treatment period (10 days). Analysis will utilize ANOVA unless statistically
significant differences in the distribution of baseline characteristics or features of
non-normality are detected and relevant, at which point contingency utilization of ANCOVA,
logistic regression, or other approaches as appropriate will be implemented. Treatment group
level rates will be presented as incidence risk ratios relative to the control (placebo)
group with 95% confidence intervals.
Safety endpoints will be evaluated on an individual AE by AE event via the DSMB and utilizing
summary statistics during treatment and through duration of follow up. Adverse events will be
presented by System Organ Class and will include information on start and stop date,
severity, projected relationship, expectedness, and outcome and duration (the latter two
after the event is considered to have concluded).
