Clinical Trial Details
— Status: Completed
Administrative data
NCT number |
NCT04602676 |
Other study ID # |
IRB_00135830 |
Secondary ID |
|
Status |
Completed |
Phase |
N/A
|
First received |
|
Last updated |
|
Start date |
November 18, 2020 |
Est. completion date |
March 5, 2021 |
Study information
Verified date |
April 2021 |
Source |
University of Utah |
Contact |
n/a |
Is FDA regulated |
No |
Health authority |
|
Study type |
Interventional
|
Clinical Trial Summary
This is a randomized crossover study, where clinicians will be randomized to periods where
they will use a rehydration calculator application with or without the Diarrheal Etiology
Prediction (DEP) algorithm. The crossover will include a washout period to reduce carryover
effect. The study will be conducted over a 9-week period. The Investigators will use a random
number generator to randomize clinicians to DEP (use of the etiology calculator) or control
arm (use of a previously-tested rehydration calculator) within site for the first 4 weeks.
After the first 4 weeks, there will be 1-week washout period without decision support, after
which each clinician will cross-over to the other arm for the next 4 weeks.
The Investigators will enroll diarrhea-treating clinicians who treat children presenting with
acute diarrhea at sites in Bangladesh and Mali. Utah investigators will only analyze
de-identified data provided by our collaborators in Bangladesh and Mali.
Description:
Diarrhoeal diseases are a leading cause of morbidity and mortality in children worldwide,
with an estimated one billion cases and 500,000 deaths annually. While the majority of deaths
due to diarrhoea occur in lower-income countries, infectious diarrhoea remains a significant
problem in high-income countries. Aside from the immediate morbidity, potential long-term
sequelae of diarrhoea in children in low-resource settings include malnutrition, growth
faltering, and deficits in cognitive development.
While the cornerstone of diarrhoeal disease management in children is rehydration, a number
of other management decisions, including the use of antibiotics and laboratory testing, may
impact the course of disease. Overuse of antibiotics may cause side-effects and lead to
increased antimicrobial resistance in the community. Underuse of antimicrobials for some
bacterial and protozoal pathogens may lead to prolonged duration of illness and facilitate
transmission. This can result in increased days of school or parental work missed, and among
malnourished children in resource-poor settings, potential for growth faltering or death.
Overuse of laboratory testing may have financial impact on both the patient and the
healthcare system, and underuse may delay appropriate therapy or prevent recognition of
outbreaks. Thus, accurate and cost-effective determination of diarrhoea etiology is important
for proper case management in children and for public health.
Clinical prediction rules (CPRs) help clinicians interpret clinical information and can
improve decision making. A recent systematic review showed that out of 137 studies of
conditions for which clinical prediction rules have been developed for children only 2 were
for diarrhoea, both of which are for the assessment of dehydration. Similarly, the majority
of available guidelines for pediatric diarrhoea are focused on the route, timing, and choice
of fluids for rehydration. A few studies in the past 30 years studied the use of clinical
predictors to estimate the probability of a bacterial cause of diarrhoea. However, these
studies were limited by low rates of pathogen identification, small sample sizes, use of a
single study site, and suboptimal prediction performance.
Given the lack of guidelines and effective clinical predictors, decisions for use of
antibiotics and laboratory testing are mostly empiric in nature, based on a number of "rules
of thumb" for which evidence is scant. Unfortunately, physician judgment does very poorly to
predict both need for antibiotics and correct type of testing. A recent study of children
presenting to Kenyan hospitals with diarrhoea showed that reliance on dysentery as a proxy
for Shigella infection led to the failure to diagnose Shigellosis in nearly 90% of cases.
Better tools for decision making and evidence-based guidelines regarding use of antibiotics
and laboratory testing in children with diarrhoea are clearly needed.
The majority of decisions for use of antibiotics in diarrhoeal illnesses are made
empirically. In lower- and middle-income countries (LMICs), due to cost constraints,
etiological diagnosis is rarely made, and a large number (up to 70%) of patients with acute
diarrhoea are prescribed antibiotics. However, in contrast to high resource settings,
bacterial pathogens may be very common in low resource settings. In the multicenter Global
Enteric Multicenter Study (GEMS) study, the investigators found that detection of Shigella
ranged from 16-78% of children with dysentery and 2-43% of children with watery diarrhoea. In
both high and low resource settings, inappropriate use of antimicrobials leads to unnecessary
toxicity for the individual, increased costs and an increase in antibiotic resistance in the
community. Thus, methods for guiding appropriate use of antibiotics for pediatric diarrhoea
in both high- and low-resource settings are urgently needed.
Clinical prediction rules (CPRs) are decision-making rubrics that help clinicians estimate
the likelihood of a patient outcome. A number of prominent prediction scores have been widely
adopted for clinical use. Examples include the CHADS2 score for stroke risk in patients with
atrial fibrillation, the TIMI score for mortality in patients with NSTEMI, and the CURB-65
Score for mortality in community-acquired pneumonia. Clinical prediction rules integrated
into clinical decision-making have the ability to direct clinicians towards more
evidence-based behaviors, resulting in improved care and reduction of costs. CPRs can also
reduce antimicrobial usage, as shown by the use of scores for strep pharyngitis, and linking
CPRs with testing guidance may further reduce antimicrobial usage. Thus, clinical prediction
rules have the potential to help healthcare workers worldwide address clinical uncertainty
and provide improved care for children with diarrhoea.
The investigators have recently use data from GEMS to derive a viral etiology prediction rule
with an internal cross-validated area under the curve (AUC) of approximately 0.85. The
investigators used a post-test odds formulation method, which takes into account odds from
multiple models or tests. First, using data from GEMS, the investigators trained a logistic
regression model with viral etiology as dependent variable using the five most predictive
clinical variables as independent variables. The investigators then trained models with the
same viral etiology response using both local climate and recent clinical trends as
independent variables. For each model, odds of viral etiology versus other known aetiologies
are generated by estimating the conditional distribution of training predictions using kernel
density estimates. The odds generated for each model are multiplied along with a pre-test
odds to determine an overall odds of a viral etiology. The investigators have now transferred
the calculation of this prediction rule into a smart-phone application, called the Diarrheal
Etiology Prediction (DEP) algorithm. The investigators have used TAC data from the VIDA
(Vaccine Impact on Diarrhea in Africa) study to externally validate the DEP algorithm's
ability to predict viral etiology of diarrhea. In this application, our objective is to
determine the acceptability and use of the DEP among clinicians caring for children with
diarrhea.