Clinical Trial Details
— Status: Completed
Administrative data
| NCT number |
NCT04491734 |
| Other study ID # |
1001 |
| Secondary ID |
|
| Status |
Completed |
| Phase |
N/A
|
| First received |
|
| Last updated |
|
| Start date |
June 1, 2020 |
| Est. completion date |
August 26, 2021 |
Study information
| Verified date |
August 2021 |
| Source |
ISOThrive Inc. |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
This is a remote study. No office visits required. The purpose and efficacy endpoint of this
study is to assess whether GERD patients tolerate ISOT-101. In addition, usage of the ReQuest
validated questionnaire to measure GERD symptoms will be explored as well as usage of the
validated SF-36 quality of life (QoL) questionnaire. Each subject serves as his/her own
control. Relative tolerability in subjects both on and off proton pump inhibitors (PPIs) will
be compared. Subjects naive to PPIs, currently taking PPIs and historically on PPIs will be
evaluated with ReQuest and QoL scores. In addition, survey measurements will be taken on a
subset of 10 subjects that are non-responders to PPIs. These will not be included in the
statistical analysis with the above groups. A tertiary endpoint of this study is to assess
any relevant adverse events that occur.
Description:
Introduction and Background GERD is found in about one-third of the population of the USA.
About 20 to 45 million people have been diagnosed by a doctor and have been prescribed daily
acid reducing medications called proton pump inhibitors (PPIs), which are the mainstay of
medical therapy for GERD. PPIs don't cure GERD and many patients take them indefinitely for
adequate symptom control. In addition, clinicians and researchers have identified concerns
with regard to chronic PPI use and the resulting possible adverse effects due to chronic
diminished gastric acid production. The potential adverse effects with reasonable association
to PPIs include osteoporosis, fractures, pneumonia, C. difficile colitis, small intestinal
bacterial overgrowth (SIBO), hypomagnesemia, vitamin B-12 deficiency, and iron deficiency
anemia. The frequent claims of potential PPI adverse effects that appear in public media has
also worried patients. In a recent article, 46% of patients on PPIs want to discontinue them
and 39% unfortunately have tried to do so without medical advice, increasing the risk of GI
bleeding, Barrett's esophagus and esophageal adenocarcinoma. Other patients, such as those at
risk for C. difficile infection, osteoporosis (the elderly), patients with small intestinal
bacterial overgrowth, among others, should not be on PPIs indefinitely. Unfortunately, there
has been no reliable cure or adequate alternative that does not share adverse effects.
ISOThrive has produced a proprietary digestion-resistant carbohydrate, ISOT-101, a specific
formulation of maltosyl-isomalto-oligosaccharides (MIMO), that serves as a prebiotic, feeding
selected bacteria that commonly inhabit the human GI tract. MIMO has an FDA Generally
Recognized As Safe (GRAS) status. Since the dawn of agrarian societies, grains were converted
to bread using a sourdough fermentation process. MIMO molecules are generally found in such
breads. These forms of breads and other sources of MIMO have been inadvertently removed from
the daily diet and so can no longer feed selective bacteria that may have played a protective
role for prior generations.
Study Rationale This is a remote study. No office visits required. The purpose and efficacy
endpoint of this study is to assess whether GERD patients tolerate ISOT-101. In addition,
usage of the ReQuest validated questionnaire to measure GERD symptoms will be explored as
well as usage of the validated SF-36 quality of life (QoL) questionnaire. Each subject serves
as his/her own control. Relative tolerability in subjects both on and off proton pump
inhibitors (PPIs) will be compared. Subjects naïve to PPIs, currently taking PPIs and
historically on PPIs will be evaluated with ReQuest and QoL scores. In addition, survey
measurements will be taken on a subset of 10 subjects that are non-responders to PPIs. These
will not be included in the statistical analysis with the above groups. A tertiary endpoint
of this study is to assess any relevant adverse events that occur.
Study Design The test material is ISOT-101. It is an approximately 90% pure
maltosyl-isomalto-oligosacchride (MIMO) prebiotic syrup produced by bacterial
fermentation/bio-conversion of sucrose and maltose. It is taken 1g daily at bedtime.
Subjects will have been previously diagnosed with GERD and will fall into one of the
following four groups:
1. Symptomatic subjects currently not taking PPI therapy and who are naive to PPIs.
2. Symptomatic subjects currently not taking PPI therapy who were responsive to prior PPI
therapy (either QD or BID) and who have been off PPIs for at least four weeks.
3. Symptomatic subjects currently taking PPI therapy (either QD or BID) who are partial
responders to PPIs.
4. 10 symptomatic subjects who have had no benefit from PPIs and have not taken PPIs for at
least 4 weeks.
All subjects will have active GERD symptoms as determined by the ReQuest validated GERD
specific questionnaire. The study has been designed to have each subject serve as their own
control so there will be no placebo arm. Each subject will receive ISOT-101 according to the
protocol. Recruitment for subjects with GERD will be by referrals from GI specialists,
primary care physicians and general advertising. Each candidate will be given information as
to how to contact the study coordinator to enroll in the study. The goal is to assess 110
subjects after the Screening Phase, including the 10 subjects who did not respond to PPIs.
All subjects will be screened per the eligibility criteria delineated in this protocol by the
study coordinator.
Two phases have been designed into this study. Phase 1 is the Screening Phase (SP). Phase 2
is the Tolerability Phase (TP). Subjects will be instructed to take a daily GERD symptom
questionnaire, the ReQuest Short Version, daily throughout the study. At five timepoints,
specific scores will be established for comparison and statistical analysis. These timepoints
are: (1) SP7 - baseline on current therapy (if any) without ISOT-101; (2) TP7 - 1 week on
both current therapy (if any) and ISOT-101; (3) TP14 - 2 weeks on both current therapy (if
any) and ISOT-101; (4) TP21 - 3 weeks on both current therapy (if any) and ISOT-101; (5))
TP28 - 4 weeks on both current therapy (if any) and ISOT-101. At each of these timepoints,
subjects will also complete the ReQuest Long Version and the SF-36 Health Survey QoL
validated questionnaires. They need not complete the ReQuest Short Version on days that the
ReQuest Long Version is required. Subjects will report any usage of all GERD medications
(PPI, H-2 antagonists, antacid) throughout their study participation.
Enrollment An adequate number of individuals will need to be screened during the Screening
Phase, using disease specific validated questionnaires to yield approximately 110 qualified
subjects to enter and likely complete the Tolerability Phase of the study. Recruitment may
involve primary care physicians and/or gastroenterologists who will make IRB approved study
information available to patients who are symptomatic for GERD. Such patients will include
those partial responders on PPI therapy; those who responded to PPIs, but have previously
stopped their PPI therapy for at least 4 weeks; those who are naive to PPI therapy, and 10
subjects that have had no benefit from PPIs and have not been on PPI therapy for at least 4
weeks. Deviations from the inclusion and exclusion criteria will not be allowed so as not to
jeopardize the scientific integrity of the study, regulatory acceptability, or subject
safety. Therefore, adherence to the criteria as specified in the protocol is essential.
All subjects will be required to sign an IRB-approved informed consent or e-consent that
complies with the requirements of both 21 CRF Part 50 and Health Insurance Portability and
Accountability Act (HIPAA) before entering the study.
The duration of the study is defined for each subject as the date a signed written informed
consent (or e-consent) is provided through Tolerability Phase Day 28. Total participation in
study may last up to 8 weeks. A comparable gender distribution is sought for the final
analysis, therefore, the ratio of male to female (or female to male) subjects completing the
Tolerability Phase will be capped at 60% of the total.
Concomitant Medications and Washout Periods GERD medications: Subjects currently taking PPI
therapy (either QD or BID) who are partial responders to PPIs may continue taking PPIs
throughout the study as needed. Subjects not taking PPIs prior to being enrolled may also
take PPIs as needed. Antacids or H-2 antagonists may be taken regularly or intermittently as
needed throughout the conduct of this study. All GERD-related medications taken by the
subject should be recorded daily via the daily electronic survey.
Prebiotic and/or probiotic supplements: Enrolled subjects must stop taking all prebiotic
and/or probiotic supplements 2 weeks prior to entering the Screening Phase of the study.
Subjects must refrain from taking prebiotic or probiotic supplements through Tolerability
Phase Day 28.
Sleep medications: Enrolled subjects taking medications for sleep disorders must be on a
stable dose at time of consent and continue at said dose through Tolerability Phase Day 28.
Antibiotics: Subjects must not have taken antibiotics within 6 months prior to signing of
consent or at any time during their participation in the study. If antibiotics are prescribed
to the subject during study participation, subject must be withdrawn from study and
discontinue daily ISOT-101 immediately.
All study product sachets (used and unused) must be returned to Investigator for product
accountability.
Subject Study Flow Process
No study-related activities will be performed and no subject data will be collected prior to
completion of the informed consent process.
Screening Phase (SP):
To enter the SP, subjects must have previously been diagnosed with GERD, be symptomatic on
their current therapy or lack of therapy, and fall into one of the 4 study groups noted in
Section 4.0 above. The SP will last for 7 days. Subjects who do not qualify at any point
during the SP will not be allowed to move into the Tolerability Phase (TP). The TP will last
28 days, beginning with first dose of ISOT-101.
Following Day 7 of SP, the average of the daily ReQuest Short Version scores will be used to
establish a baseline score to confirm that the subject is experiencing GERD symptoms. Any
subject who has a ReQuest Short Version (RQ) average score of >= 3.37 (90 percentile) or
ReQuest GI (RQ-GI) average score >=0.95 on the will be eligible to transition to the
Tolerability Phase. The ReQuest Short Version SP1-SP7 average and SF-36 will serve as a
baseline. Investigator will verify eligibility prior to study staff contacting subject.
Once eligibility has been verified by the PI, the study coordinator will inform subject and
confirm that subject wishes to continue in the study. Once confirmed, study coordinator will:
- Review concomitant medications
- Collect any adverse events
- Review calendar for remainder of study
- Provide instructions for daily dosing of ISOT-101
- Confirm mailing address
- Arrange for shipment of 30-day supply of ISOT-101 to the subject There may be up to 7
calendar days between SP Day 7 and TP Day 1 depending on length of time to ship/receive
ISOT-101.
Tolerability Phase (TP)
Subjects will take their current GERD therapy as follows:
- If on PPI therapy QD or BID, then the PPI is to be taken as the subject customarily has
taken it, prior to beginning the study.
- If on an H-2 antagonist or antacid, then the subject may continue these medications as
needed throughout the study.
All GERD medications and other medications will be recorded daily via the electronic survey.
• ISOT-101 will be taken daily at bedtime (one sachet per day). This will be the last thing
swallowed prior to bedtime (no rinsing, and after brushing teeth) As the primary endpoint,
tolerability of ISOT-101 will be assessed. In addition, changes in the ReQuest Short Version
GERD symptom scores (RQ, RQ-GI and RQ-WSO) and SF-36 scores will be assessed for all subjects
as well as for the sub-group of subjects that completed all 4 weeks of the protocol. Changes
in ReQuest symptom scores, or SF-36 scores, between time point 1 and time point 2 will be the
basis of this assessment. Further evaluation will include comparison of ISOT-101 tolerability
in the 4 subject sub-groups using these two time points.
The safety endpoint of the study is to ensure that any adverse events that are reported or
observed during the study are appropriately recorded.
