Cardiovascular Diseases Clinical Trial
Official title:
An Open Cluster-randomized, 18 Month Trial to Compare the Effectiveness of Educational Outreach Visits With Usual Guideline Dissemination to Improve Family Physician Prescribing
Background: The Portuguese National Health Directorate has issued clinical practice
guidelines on prescription of anti-inflammatory drugs and COX-2 inhibitors, acid suppressive
therapy and proton pump inhibitors, and anti-platelets. However, their effectiveness in
changing actual practice is unknown. The objectives will be to compare the effectiveness of
educational outreach visits in the implementation of clinical guidelines in primary care in
Portugal against usual implementation strategies and to conduct a cost-effectiveness
analysis of this method.
Methods: The trial will be a parallel, cluster-randomized, unblinded, trial in primary care,
with a 1:1 allocation ratio. This study will assess the effect of educational outreach
visits on physician compliance with prescription guidelines. The general study hypothesis is
whether educational outreach visits are superior to usual implementation of guidelines
regarding the reduction of inappropriate prescribing (compliance with prescription
guidelines). All National Health Service primary care units in the Lisbon (Portugal) region
will be invited to participate. Units will be eligible if they are using an Electronic
Health Record to issue prescriptions and have at least four doctors willing to participate.
Doctors in intervention units will receive three educational outreach visits (one for each
guideline) during a six months period, while the control group doctors will be offered an
unrelated group training session (on using the international classification for primary
care). Intervention visits will be one on one 15 minutes discussions conducted by guideline
authors or trained family physicians at the physician's workplace. There are two primary
outcomes, measured at the physician's level. One is the proportion of COX-2 inhibitors
prescribed within the entire NSAID class, in defined daily doses 18 months after the
intervention. The other is the proportion of omeprazole within the entire proton pump
inhibitors class, in defined daily doses at 18 months post-intervention. Prescription data
will be collected from the regional pharmacy claims database.
The trial will be a parallel, cluster-randomized, unblinded, trial in primary care, with a
1:1 allocation ratio. This study will assess the effect of educational outreach visits on
physician compliance with prescription guidelines. The general study hypothesis is whether
educational outreach visits are superior to usual implementation of guidelines regarding the
reduction of inappropriate prescribing (compliance with prescription guidelines). All
National Health Service primary care units in the Lisbon (Portugal) region will be invited
to participate. Units will be eligible if they are using an Electronic Health Record to
issue prescriptions and have at least four doctors willing to participate. Doctors in
intervention units will receive three educational outreach visits (one for each guideline)
during a six months period, while the control group doctors will be offered an unrelated
group training session (on using the international classification for primary care).
Intervention visits will be one on one 15 minutes discussions conducted by guideline authors
or trained family physicians at the physician's workplace. There are two primary outcomes,
measured at the physician's level. One is the proportion of COX-2 inhibitors prescribed
within the entire NSAID class, in defined daily doses 18 months after the intervention. The
other is the proportion of omeprazole within the entire proton pump inhibitors class, in
defined daily doses at 18 months post-intervention.Besides the above primary endpoints, the
secondary outcomes will be the short (1 month) and medium-term (6 months) effects of
educational outreach visits in the prescription of these two drug classes. Other secondary
endpoints will be the short, medium and long-term effects of educational outreach visits in
the prescription of clopidogrel. Finally, the trial will determine the cost effectiveness of
educational outreach visits.
Allocation to intervention and blinding:
Clusters will be enrolled and allocated sequentially. To achieve a good balance regarding
baseline characteristics, the allocation sequence will be determined by minimization (Ivers
NI 2012). The units will be minimized by number of doctors (4 or 5, 6 or 7, 8 to12), median
baseline prescription of COX-2 inhibitors (above or below the regional median), median
baseline prescription of omeprazole (above or below the regional median), proportion of
doctors with less than 10 years of practice after completing vocational training (above or
below 50%), and type of primary care unit (family health unit or personalized care unit).
All doctors sending the consent statement before the cluster allocation will be included in
the study.
The sequence of intervention visits for each unit will be determined by simple
randomization.
Allocation concealment will be ensured by the following procedures: the trial manager (hired
and not part of the authors research team) will assign a sequential number to each unit as
participation forms are received; only anonymized data about participating units will be
sent to the trial statistician (sequential number and minimization variables); data will be
sent in two batches, one for each half of all units; the statistician will allocate units to
each trial arm using minimization; the sequence of visits will be determined using the
random sequence generator from Random.org (http://www.random.org/sequences/); the
statistician will return allocation information to the trial manager.
Due to the nature of the intervention, neither family physicians, nor detailers can be
blinded. Outcomes are routinely collected by the regional health administration
independently of the researchers or the trial and will only be sent to researchers after the
intervention has ended. Data analysts (the trial statistician plus one of the members of the
research team) will be blinded to group and visit sequence allocation until all analysis are
completed.
Intervention and comparison:
Doctors in units randomized to the intervention will have three educational outreach visits
during a six month period. These visits will promote the implementation of governmental
guidelines on the prescription of the following agents: non-steroidal anti-inflammatory
drugs (NSAIDs) and COX-2 inhibitors, acid secretion modifiers, and antiplatelets. The
outcomes for the trial were chosen according to the main key-message from each guideline.
For NSAIDs, COX-2 inhibitors should be prescribed only in patients with increased
gastrointestinal risk who do not tolerate a classical NSAID associated with a
gastroprotective agent; for acid secretion modifiers, all proton pump inhibitors are
equivalent in effectiveness so omeprazole should be used in most patients as it is the least
expensive; for antiplatelets, there is no benefit of maintaining long term clopidogrel after
a myocardial infarction, acute coronary syndrome or percutaneous coronary intervention.
Intervention group: During each 15 to 20 minutes visit an academic detailer will promote one
of the guidelines to a family doctor (up to three physicians may be present in each visit if
they wish to, but one to one visits will be preferred and encouraged). The detailer will
also distribute a point of care summary highlighting the main messages.
Control group: Usual guideline implementation consists of passive dissemination by their
publication on the National Health Directorate's website. Doctors in units randomized to the
control group will be offered an unrelated training session (coding with the International
Classification of Primary Care, second edition) as a token of good will for participating in
the trial.
Cost analysis:
Global prescription spending will be defined as the sum of the cost of all drug
prescriptions of NSAIDs (ATC M01A), acid suppressive therapy (proton pump inhibitors ATC
A02BC and their alternatives: H2-receptor antagonists ATC A02BA, antacids ATC A02A,
misoprostol ATC A02BB01, and sucralfate ATC A02BX02), and antiplatelets (ATC B01AC) , up to
18 months after the intervention. These costs will be compared with the amount spent
training the detailers, preparing and printing educational materials, travel expenses to
intervention units, payment of detailers, program coordination, and physician time spent
with a detailer rather than with a patient. Costs will be analyzed from the point of view of
an educational outreach program rather than from conducting research. Therefore research
related costs (such as researcher time for data collection and analysis) will not be
considered. Similarly, the unrelated training session offered to the control units will not
be accounted for because it is only intended to improve recruitment and it would not be
necessary for the implementation of an educational outreach program.
Data collection:
Researchers will have access to prescription data through a data monitoring system operated
by the Regional Health Administration. Data will be collected and provided by employees from
this Administration according to researcher defined specifications. Importantly, researchers
will not be directly involved in data collection. This information arrives with a two month
delay from the date the prescription is dispensed. The prescription information contained
there can be either for acute conditions - single prescriptions with up to two packages to
be dispensed within 30 days; or for chronic usage - three identical prescriptions (up to two
packages each) to be dispensed within 6 months. Within the drug classes of this study, only
NSAIDs cannot be prescribed for chronic usage. Adverse events cannot be collected in this
study because only prescription data is available.
Detailers will record whether the planned visit was effectively accomplished, whether it had
the planned duration, the number of physicians (including residents) present, whether the
visit was made on patient visit time or off hours, the number of times the detailer had
previously visited that physician, and feedback from the physician about the educational
materials.
Sample size:
The research team has obtained pilot data from all physicians of three primary care units.
This data was used to estimate within unit variability and the intra-cluster correlation
coefficient (ICC). Data was also gathered for all the units in the Regional Health
Administration to estimate the mean prescription and standard deviation for the primary
outcomes. The mean proportion of omeprazole dispensed was 54.0% of all PPIs (standard
deviation, SD, 10.1%) and the ICC was 0.027. The mean proportion of COX-2 inhibitors
dispensed was 20.6% of all oral NSAIDs (SD 7.4%) and the ICC was 0.249. The Cochrane review
on educational outreach visits found a median adjusted risk difference for improvement in
compliance with desired practice of 5.6% (interquartile range 3.0% to 9.0%) in previous
trials (O' Brien, 2008). Therefore, we chose to calculate our sample size assuming the
intervention would lead to about 5% absolute difference between intervention and control
units.
If one assumes a mean cluster size of 6 doctors per unit, a 1:1 allocation ratio of controls
per intervention unit, an alpha type error of 0.025, and a dropout rate of about 15%, then a
sample of 110 doctors in each group will allow for 80% power to demonstrate a 5% absolute
increase in the proportion omeprazole and a 5% absolute decrease in COX-2 inhibitors. To
recruit the necessary number of physicians about 38 primary care units will be required.
STATA 12.0 (STATA Corp, TX, USA) and its sampsi and sampclus commands were used to calculate
sample size.
Statistical methods:
Physicians will be analyzed according to their randomly allocated group regardless of
adherence to the intervention (intention to treat analysis). If physicians transfer to
another unit within the health region we will still be able to monitor their prescriptions.
If the transfer is to a different health region (i.e. not the Lisbon one) we will contact
the physician and ask for the missing prescription data. In both cases, prescription of
clopidogrel will be adjusted to the new patient list. If a physician retires or we are
unable to retrieve data from a physician who moved to a different region then we will use
the last working month's prescription.
Both groups will be compared on primary outcomes using a generalized mixed-effects model.
The ratio of COX-2 inhibitors to the entire NSAIDs class and the ratio of omeprazole to the
entire proton pump inhibitors class and respective 95% confidence intervals will be
calculated. Statistical significance will be assumed for a p-value of less than 0.025. STATA
12.0 (STATA Corp, TX, USA) will be used to conduct the analysis.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Health Services Research
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