Helicobacter Pylori Infection Clinical Trial
Official title:
Eradication of Helicobacter Pylori With a Lactobacillus Reuteri Strain Combination (Strains DSM 17938 and ATCC PTA 6475) and a Proton Pump Inhibitor
Meta-analyses involving >4000 subjects with probiotics added to antimicrobial Helicobacter
pylori eradication therapy in populations with antibiotic resistance have reported a mean
increase in eradication rate of 12.2%. It is unclear how to translate that result into
clinical practice.
To evaluate whether administration of Lactobacillus reuteri plus a PPI without antibiotics
would eradicate H. pylori infections.
This was a double-blind placebo-controlled randomized 2 site study of L. reuteri (2 x 108 CFU
L. reuteri DSM 17938 plus 2 x 108 CFU L. reuteri ATCC PTA 6475) 7 times per day or matching
placebo plus 20 mg pantoprazole b.i.d. for 4 weeks. Cure was defined by negative 13C-UBT, 4
weeks after therapy. Sample size was based on obtaining >50% cures to be clinically useful as
monotherapy.
Aim of study This double-blind study will assess if the combination of PPI and a strain
combination (Gastrus) of L.reuteri can yield higher eradication rates if doses are increased
and dose interval shortened. The aim is to achieve at least 50% eradication as assessed by
UBT.
Study Product
Gastrus capsules:
2x108 CFU Lactobacillus reuteri DSM 17938 + 2x108 CFU Lactobacillus reuteri ATCC PTA 6475.
Placebo capsules:
Identical in shape, colour and taste to Gastrus capsules but without the Lactobacillus
reuteri components.
Both study products are delivered in identical containers containing 30 capsules.
Dosing Group 1: 1 Gastrus capsule 7 times per day + Pantoprazole 20 mg b.i.d. Group 2: 1
placebo capsule 7 times per day + Pantoprazole 20 mg b.i.d. One capsule of the Study Product
are to be taken every 2-3 hours 7 times per day.
The Study Product containers will be collected at the day 28 visit and remaining tablets are
counted and compliance checked.
40 mg Pantoprazole is to be taken just before breakfast and dinner (i.e. daily dose 80 mg).
Length of treatment The optimal length of dosing needed is unknown. Saggioro and Francavilla
used 30 and 28 days respectively and Dore et al had a 60-day regimen. From a
practical/economical/tolerability point of view, a 28-day regimen is suggested in order to
shorten the time to triple-therapy for those non-eradicated. Those patients with H. pylori at
the second UBT/Endoscopy (i.e. treatment failures) will be offered standard eradication
therapy.
Compliance, PP and ITT In order to be assessed as "compliant" the participant should have
consumed at least 75% (or other?) of the allotted doses. In order to improve compliance, the
participants will be equipped with alarm-devices. Compliant patients will be assessed as
Per-Protocol (PP). Patients that are non-compliant but have consumed at least one full day of
doses (i.e. 14 tablets) will be included in the Intention-To-Treat analysis.
Outcomes Primary efficacy parameter Number of H. pylori-eradicated at 9 weeks as evidenced by
Δ-13C-UBT < 5 ppm. The difference between active and placebo treatment will be compared.
Exploratory parameters Changes in GSRS at 4 and 9 weeks as compared to baseline and between
groups. Changes of the gastric microbiota in the presence of PPI with or without Gastrus.
Sample size calculation Assuming that the spontaneous eradication is 5% or less, and that the
desired eradication rate on active treatment is >50%, 23 subjects are needed in each group
with a power of 90% and a confidence level of 95%. To correct for potential drop-outs, 25
subjects will be recruited to each group.
Ethical committee The study protocol will have to be approved by the local ethical committee
before study start. Once approved, a protocol summary will be posted on clinicaltrials.gov.
Study flow and procedures Randomisation & labelling Randomisation will be computerised using
the tool provided by randomizer.org. A third party not otherwise involved in the study will
label active and placebo Study Product. Randomisation lists will be kept in sealed envelopes
at the study sites and a sealed copy will also be kept at BioGaia. The envelopes may not be
open until all study data have been entered into the database and until the database has been
locked. However, see "Serious Adverse Event" below.
Patients will be entered into the study sequentially by allocating the lowest available
remaining randomisation number to the patient.
Procedures Histology During endoscopy two biopsy specimens are taken from the antrum, one
from the angulus and two from the corpus. Hp-infection is defined as the presence of typical
histology and bacteria on histological examination of biopsies stained by H&E and GIEMSA. One
additional biopsy from the corpus area is placed in PBS with 5% glycerol and stored at - 70
oC until further processing for microbiota analyses (see below.
Gastric microbiota analysis Bacterial DNA extraction and sequencing for microbiota analyses
is performed according to a standardised protocol (Willing BP et. al 2010). Analysis of
community structure focuses on sequencing of targeted regions e.g. the 16S rRNA gene using
the Illumina Miseq high-throughput sequencing platform. Sequences are finally processed with
the QIIME 1.8.0 pipeline (Caporaso JG et. al 2010).
13C-UBT According to standard protocol (Gatta L., et al. 2006). After the first UBT needed
for inclusion, a second UBT will be performed at 8-9 weeks (4-5 weeks after end of study
treatment) to assess Hp status.
Gastrointestinal Symptom Rating Scale (GSRS). Participants will be asked to fill out the GSRS
questionnaire after inclusion but before taking the first dose of study product, at 4 weeks
(end of treatment) and at 8-9 weeks (at follow-up UBT) (Svedlund J. et al. 1988) Data
collection The Principal Investigator will prepare one set of Case Record Forms (CRF) for
each patient in which all data pertinent to the study will be entered.
Statistical methods All efficacy parameters will be analysed according to both ITT and PP.
Safety considerations The investigator is responsible for monitoring the safety of subjects
who have entered the study. All adverse events (AE) occurring after any administration of the
study product will be followed to the end of the study or until resolution. AE will be
evaluated by the Investigator and reported in the CRF.
Serious adverse events, as defined below, must be reported to the sponsor within 24 hours of
when the investigator became aware of the SAE. It is also important to report all adverse
events that result in permanent discontinuation of the study product, whether serious or
non-serious.
Adverse Events An adverse event (AE) is any undesirable medical occurrence in a subject
administered a study product, regardless of causality assessment. An adverse event can
therefore be any unfavourable and unintended sign (including an abnormal laboratory finding),
symptom, or disease temporally associated with the use of a study product, whether or not
considered related to the study product. All adverse events, including observed or
volunteered problems, complaints, or symptoms are to be recorded on the case report form
(CRF). Each adverse event is to be evaluated for duration, intensity, and causal relationship
with the study product or other factors.
Subjects should be instructed to report any AE that they experience to the Investigator.
Investigators should assess for AE at each visit. AE occurring during the clinical trial,
including the follow-up period should be recorded on the appropriate AE CRF. To capture the
most potentially relevant safety information during a clinical trial, it is important that
investigators record accurate AE terms on CRF.
If discernible at the time of completing an AE in CRF, a specific disease or syndrome rather
than individual associated signs and symptoms should be identified by the investigator and
recorded on the CRF. However, if an observed or reported sign or symptom is not considered a
component of a specific disease or syndrome by the investigator, it should be recorded as a
separate AE on the CRF. Laboratory values will be collected on the laboratory CRF. Do not
enter changes from baseline in laboratory values on the AE CRF.
Serious Adverse Events A serious adverse event (SAE) is any AE that results in death is
immediately life threatening requires or prolongs hospitalisation results in persistent or
significant disability/incapacity is a medically significant event for any reason. Breaking
the randomisation code In case that the responsible investigator decides that the
randomisation code has to be revealed because that the AE may have been caused by the Study
Product and that un-blinding is of essence for the further treatment of the patient, the
following procedure will be followed: The responsible investigator will assign a professional
otherwise not involved in the study to un-blind the Study Product for the specific patient.
He/she will open the sealed envelope, find the relevant randomisation number and inform the
responsible investigator without revealing any other randomisation numbers. He/she will then
re-seal the envelope with transparent tape, date and sign on the tape.
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