Gastroesophageal Reflux Disease Clinical Trial
Official title:
Impact of Head of Bed Elevation in Symptoms of Patients With Gastroesophageal Reflux Disease: a Randomized Single-blind Study
BACKGROUND: Gastroesophageal reflux disease is a very frequent clinical condition and
nocturnal symptoms are a cause of quality of life impairment, poor sleep quality and
absenteeism. Head of bed elevation, as a low-cost non pharmacologic anti-reflux treatment is
nowadays recommended, but its clinical impact in patients with nocturnal symptoms remains
unknown due to inconsistent results and methodological limitations among different clinical
trials, most of which were performed before the widespread use of proton pump inhibitors in
clinical practice.
HYPOTHESIS: Head of bed elevation is a useful treatment for patients with gastroesophageal
reflux disease and nocturnal symptoms, and has a positive impact in quality of life in these
patients.
STUDY OBJECTIVE: To assess the effectiveness of head of bed elevation for treatment of
patients with gastroesophageal reflux disease and nocturnal symptoms, and to determine the
impact of this intervention in quality of life of these patients.
METHODS: Randomized single-blind single-centre controlled clinical trial with a 2x2
cross-over design. A sample of 42 patients attending to the outpatient gastroenterology unit
at Clínica Fundadores in Bogotá city, who met the inclusion criteria and had no exclusion
criteria were selected to participate. Included patients were randomized to raise the head of
bed with standard 20 cm-height wooden blocks or to sleep without bed inclination during the
first 6 week period. After a 2 week washout period, allocation was crossed and participants
were followed again during a second 6 week period. During the trial, every patient received
standard pharmacological treatment with a proton pump inhibitor and/or sodium alginate. After
allocation concealment, the researchers in charge of statistical analysis and reporting
results were blinded for the non pharmacological intervention under study. Primary outcome
was a significant symptom change according to Reflux Disease Questionnaire (RDQ) validated
form. Secondary outcomes include impact on quality of life according to Short Form 36 (SF-36)
validated questionnaire, patient preference and adverse events of non-pharmacological
intervention. Statistical analysis was carried out with STATA 13.0 (Special Edition) for
Windows. Differences with a p<0,05 were accepted as statistically significant.
PROBLEM STATEMENT
Gastroesophageal reflux disease (GERD) is a clinical condition characterized by troublesome
symptoms and medical complications as a result of reflux of gastric contents into the
esophagus. GERD is diagnosed in 4% of primary care outpatient visits and the disease
prevalence in Latin-America reaches 12-31%. Nocturnal symptoms have been found in 74% of
patients with GERD and are a cause of significant quality of life impairment, when compared
with general population and patients with GERD and daytime-only symptoms. Sleep interference
secondary to nocturnal retrosternal burning has been associated to lower work productivity,
even in patients being treated with proton pump inhibitors (PPI). Due to several
physiological factors such as lack of conscious perception of symptoms, reduced salivation
and a lower frequency of nocturnal swallowing, a significantly longer acid exposure overnight
has been associated to the emergence of complications like esophagitis, more extra-esophageal
symptoms and other illnesses such as asthma.
As a low-cost non pharmacological anti-reflux treatment for GERD, head of bed elevation (HBE)
is nowadays a moderate-strength recommendation with low level of evidence. Clinical impact of
this measure in patients with night-time symptoms remains unknown, due to inconsistent
results and methodological limitations among different clinical trials; most of which were
performed before the widespread use of proton pump inhibitors in clinical practice. Evidence
from several non-randomized studies suggest that HBE could reduce esophageal acid exposure
time and could decrease GERD symptoms; however, another study found no significant
differences in those same outcomes. On the other hand, all randomized controlled clinical
trials published this far show inconsistent results. A study published before widely accepted
clinical use of PPI, revealed significant clinical and endoscopic improvement with HBE in
patients with GERD and grade C-D esophagitis, when compared to controls. In contrast, a
multi-centre clinical trial found no difference in symptom score or antacid use among groups
allocated to HBE and control group. All cited studies have methodological limitations and
heterogeneity in outcome assessments, which makes difficult conducting a meta-analysis with
these data. No published studies evaluating impact of HBE in quality of life or work
productivity were found.
SAMPLE SIZE CALCULATION
Sample size was estimated based on the hypothesis that HBE would produce a difference of at
least 10% in RDQ and SF-36 scores. Effect size (Cohen d) was calculated as 0,49, keeping in
mind an RDQ mean and standard deviation of 3,3±1,0 previously found in Spanish population
with symptomatic GERD. An SF-36 mean and standard deviation of 56,9±20,3 reported in Italian
population in medical therapy with PPI were also taken into account. The minimally important
difference selection was chosen based on the assumption that any difference smaller than 10%
would have no clinical relevance. Based on this data, 14 patients per group would yield a
power greater than 80% for detection of a minimally important difference as large as or
larger than 0,6 points in RDQ questionnaire (range: 1 to 6) and 10 points in SF-36
questionnaire (range: 0 to 100), when using a paired t test. For a complementary analysis of
this trial, by using a McNemar test, effect size was recalculated based on published clinical
trial data from pre-omeprazole era, according to which 58,8% and 28,6% of patients assigned
to placebo improved gastroesophageal reflux symptoms with and without 20 cm HBE,
respectively. Based on this data, and maintaining a statistical power of 80%, required sample
size was adjusted to a total of 34 patients. G*Power 3.1.9.2 software (Universität
Düsseldorf, Düsseldorf, Germany). Finally, estimated sample size was incremented by 20% to
avoid that eventual losses of follow-up may alter study power. Therefore, final sample size
was 42 patients, 21 patients per group.
DESIGN AND CARVING OF WOODEN PRISMS
84 prisms of withered pine tree wood with dimensions 20x18x18 cm were carved from 9 logs of
300x20x20 cm at Aserrío San Ignacio Ltda. production plant, located in Soacha, Cundinamarca.
Given it is an industrial process of chainsaw cutting and wood planing, a quality control was
implemented consisting of verification of prism stability while lying on the floor, and the
mean height in millimeters of every prism will also be measured and registered. Unsteady
products or those with atypical mean heights, defined as a height either exceeding percentile
75 + 1,5 times interquartile range or below percentile 25 - 1,5 times interquartile range,
will be discarded and not used during the study. After exclusion of defective prisms,42
groups of wooden prism pairs according to mean height in millimeters were formed and every
group was given a random digit generated by computer. Afterwards, every random digit of prism
groups was sequentially assigned to a consecutive HBE-allocated patient number, in such a way
that every consecutive patient number (among those allocated to HBE) will be linked randomly
to a preset known prism height. This additional randomization procedure involving prisms
according to their mean height, is planned due to the impossibility to guarantee that prism
height will be identical with a precision of ±1 mm, keeping in mind that products will be cut
with chainsaw and will be planed as part of an industrial process. After quality control
process, mean prism height was found to be a non-normal distributed variable (W:0,908; critic
W: 0,979; p: 0,000000), and after applying predetermined exclusion rules for atypical data, 2
pairs of wooden prisms were discarded.
RANDOMIZATION
A random binomial number list (zeroes and ones) will be generated with the statistical
software STATA SE 13.0 for Windows and the list will be used for allocation of 42 patients
between intervention and control groups in a 1:1 proportion. Each one of the 42 pairs of
wooden prisms will be marked with a consecutive number coming from an HBE-allocated patient
and the prisms will be stored keeping the marked number out of reach from the sight of the
researcher in charge of patient recruiting.
Patients that meet the inclusion criteria, have no exclusion criteria and who give written
informed consent, will be assigned a consecutive number during their outpatient visit
according to their order of inclusion in the trial. These participants will be randomized to
either HBE or control group in the moment that a member of the research team verifies, among
the stored prisms, the existence of a prism pair marked with the same number as the
consecutive number assigned to the patient. In the case that this pair does exist, then the
patient will take home that pair of wooden prisms and use them during the first period of the
trial according to spoken and written instructions to be given at that moment. On the
contrary, if a pair of wooden prisms marked with the same consecutive number as the patient,
does not exist, then it will be understood that the study participant has been allocated to
control group during the first period of the trial. The member of the research team who
verifies the storehouse of wooden prisms will not be in charge of confirming inclusion and
exclusion criteria and will not assign consecutive numbers to patients during outpatient
visits.
ALLOCATION CONCEALMENT
The researcher in charge of confirming inclusion and exclusion criteria, fulfilling the Basic
Data Formulary and providing the patient with the Informed Consent Format, will not be aware
of the allocation sequence order until these 3 documents have been applied to the participant
and a consecutive number has been generated according to their order of inclusion in the
trial. After that, a member of the research team in the prism storehouse will verify the
existence of a prism pair marked with the same number as the consecutive number assigned to
the patient, and only in that point allocation status of the participant will be known.
CROSS-OVER
After allocation has been completed, patients in the intervention group will receive a pair
of numbered wooden prisms with dimensions 20x18x18 cm along with written instructions about
the correct use of the intervention. The patient must sleep with HBE during 6 weeks and both
RDQ and SF-36 questionnaires will be applied again at the end of this first period while the
participant is still sleeping with HBE. Afterwards, a washout 2 week period follows in which
the participant sleeping with HBE will stop using it and will return the pair of wooden
prisms to the researchers. After washout period has ended and both RDQ and SF-36
questionnaires have been applied again, patients allocated to the control group during the
first period of the study will receive a random pair of prisms and will be instructed to use
the prisms for sleeping with HBE during a second period of 6 weeks. Meanwhile, participants
initially allocated to the HBE group will be followed as a control group in this second
period of the study.
FOLLOW-UP
After participant allocation, telephonic follow up will be made during both periods of the
trial with a frequency that is dependent on the intervention group of the patient in that
period. Participants in the HBE group will be called weekly for 2 weeks, and then will be
called biweekly for a month, until each period of 6 weeks has ended. In contrast, patients in
the control group will be called every three weeks along each period. With the purpose of
verifying both HBE adherence and correct use of wooden prisms, every participant will be
asked to send a photograph of the bed head legs during the follow-up telephone call. The
photograph will be received by the researcher via e-mail or smart-phone and will be encoded
and saved in a hard disk. At the end of the first period, RDQ and SF-36 questionnaires will
be applied and researchers will store the returned prisms during washout period. When washout
period has ended, RDQ and SF-36 questionnaires will be applied again in order to be sure of
the absence of any carry-over effect in the group initially allocated to HBE. Finally at week
14, RDQ, SF-36 and Patient Preference questionnaires will be administered to complete study
ending outcome assessments.
STATISTIC ANALYSIS PLAN
Quantitative and qualitative variables collected with Basic Data Format, RDQ, SF-36 and
Patient Preference questionnaires will be typed in a Microsoft Excel 2007 database.
Intervention groups will be masked with an alphabetical code provided by an independent
collaborator who will not be involved with data analysis or report writing. For statistical
processing, database will be imported into STATA SE 13.0 for Windows and descriptive
statistics will be generated for each variable. Statistically significant differences will be
searched for categorical data using the Chi-square test and normality will be tested for
numerical continuous variables using the Shapiro-Wilk test. For normally distributed
continuous variables, statistically significant differences will be searched for by using
unpaired Student's t test. Alternatively, for not normally distributed variables a Wilcoxon
signed rank test will be applied. For complementary processing of primary outcome and
secondary outcome quality of life, score difference between periods will be transformed into
a binomial variable and a McNemar test will be applied. Differences with one-tail p<0,05 will
be accepted as statistically significant. Subgroup analysis will explore differences
stratified according to age group, sex, ethnic group, BMI, comorbidities, cups of coffee per
day, pharmacological adherence, and length and severity of symptoms.
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