Acute Gastroenteritis Clinical Trial
Official title:
A Case-Control Study to Assess the Effectiveness of Rotarix Vaccine (RV1)
To determine the effectiveness of rotavirus vaccines, active surveillance will be conducted
at two sites, Cincinnati Children's Hospital Medical Center (CCHMC) in Cincinnati, Ohio and
the Medical University of South Carolina (MUSC) in Charleston, South Carolina.
Children born on or after April 1, 2006 presenting to CCHMC as an inpatient or for a
short-stay or Emergency Department (ED) visit with acute gastroenteritis (AGE) and/or fever
will be approached for enrollment. Children will be eligible if they have vomiting and/or
diarrhea less than or equal to 10 days duration. Data including demographic information,
illness characteristics and socio-economic status will be collected from each patient. A
sample of the patient's stool will be collected within 14 days of the onset of symptoms.
Stool specimens will be tested for rotavirus antigen by Rotaclone at CCHMC. All rotavirus
positive stool specimens will be typed for common G and P serotypes. Using the children
identified with rotavirus as our cases and the children who were rotavirus negative as our
controls, we will conduct a case control study to assess the effectiveness of rotavirus
vaccines, in particular Rotarix.
A case-control design will be utilized to assess the effectiveness of RV1 in preventing
rotavirus-associated hospitalizations and Emergency Department (ED) visits using cases and
controls from the 2009-2012 rotavirus seasons. Vaccine exposure among cases will be compared
to vaccine exposure among controls. There will be one case group and one control group.
Cases will be obtained from children who are enrolled in active surveillance for acute
gastroenteritis being conducted at the two initial surveillance sites. These sites include:
Cincinnati Children's Hospital Medical Center (2009-2012) and the Medical University of
South Carolina (2009-2012). Cases and controls will be identified retrospectively for the
2008-2011 seasons and prospectively through active surveillance for the 2011-2012 season.
The active surveillance programs conduct prospective surveillance for hospitalizations and
ED visits due to AGE (acute gastroenteritis) in children < 6 years of age. Even though
Rotarix was commercially available on January 1, 2008, the actual date that RV1 was
initially used varied across sites. The date that Rotarix was initially used will be
determined for each site through examination of the data. Children with laboratory-confirmed
rotavirus infection (bulk stool sample positive for rotavirus using a rotavirus EIA) will be
included as a case if they were born 2 months prior to the initial date of Rotarix
availability at each site. The vaccine record for each case will be obtained to determine
the vaccine status of the child.
Controls will be children born 2 months prior to the availability of Rotarix at each site
who were enrolled in the active surveillance program at either site and who tested negative
for rotavirus. Children who have been previously hospitalized for diarrhea, who have a
sibling enrolled in the study, or who have recently moved into the study area (and might not
have been eligible for the vaccine) will be excluded.
Laboratory Testing
For children enrolled in the active surveillance program bulk stool specimens are obtained
within 14 days of the visit for AGE symptoms and are tested using Rotaclone, a commercial
enzyme immunoassay (Meridian Bioscience, Inc) at CCHMC. Children with a positive test for
rotavirus are eligible to be cases and children with a negative test for rotavirus are
eligible for controls. Specimens positive by EIA for rotavirus will have G and P genotyping
done at CCHMC.
Retrospective Enrollment of Children Tested for Rotavirus as Part of Routine Care
With the dramatic decline in rotavirus since the introduction of rotavirus vaccines, the
number of children enrolled in surveillance has plummeted compared to pre-licensure
surveillance. In order to improve our sample size, we will retrospectively invite children
who had a rotavirus test done from August 1, 2008 through June 30, 2012 to participate in
this study. The laboratory records of rotavirus testing will be reviewed to identify
children with a date of birth >August 1, 2008. Once identified, a letter will be sent to the
parents/guardians with a brief explanation of the study and we will ask them to notify us
within two weeks if they do not wish to be called. Study staff will then contact the
parent/guardian to explain the study and to determine whether the child meets eligibility
criteria (same as those outlined for enrollment into surveillance). If the child meets
eligibility criteria, the parents/guardians will be asked to allow their child to
participate, informed consent will be obtained for the child. If agreed, the same data
collected on prospectively enrolled children will be collected and permission will be
obtained to contact the child's health care provider for the child's immunization records.
Eligibility
The date that Rotarix was initially used will be determined for each site. Children born 2
months prior to the initial date or later will be eligible to be a case or control for this
study. If a child is enrolled more than once during the same season, the visit at which the
child tested positive for rotavirus will be selected for inclusion; if the child tested
negative at all visits, the child's final visit will be selected for inclusion.
Sample Size
Sample size calculations were done for varying degrees of vaccine efficacy and vaccine
coverage. With a vaccine uptake of 20%, 68 cases would allow a detection of vaccine
effectiveness of 80% assuming a two-sided test with a significance level of 0.05 and 80%
power. If the vaccine uptake is 30% only 44 cases would be needed to detect a vaccine
effectiveness of 80%.
One must take into consideration that both cases and controls may have incomplete
immunization series. If there are a sufficient number of cases, one dose vaccine efficacy
will also be examined.
Statistical Analysis
Analyses will be performed using SAS® (Version 9.2 Cary, NC). Demographic and risk factor
variables will be examined. Continuous, parametric data will be presented as mean ± standard
deviation (SD); continuous, non-parametric data will be presented as median (inter-quartile
range). Categorical data will be presented as frequency (percentage) by category.
Continuous, parametric data will be analyzed with ANOVA or Student's t-test. Categorical
data will be analyzed with chi-square or Fisher's Exact Test as appropriate.
Logistic Regression will be used to estimate Vaccine Effectiveness (VE) and 95% confidence
intervals (CIs) from the adjusted odds ratios (aORs) by using the formula VE = (1-aOR) X
100. Cases and controls will be matched on age, enrollment date, and geographic region.
Cases will be compared to matched controls in order to evaluate the effectiveness of full (2
doses) and partial (1 dose) vaccination. Initially, univariate conditional logistic
regression analyses will be performed to determine which covariates should be included in
the multivariable analysis. The explanatory variable of interest is vaccination status. If
sample size permits, vaccine effectiveness will be calculated by serotype. Other possible
covariates to be included are: date of birth, age at onset, season, insurance status
(public/none versus private) and point of care (hospital or ED). Variables with p-values ≤
0.20 will selected as candidates for multivariable analysis. Multicollinearity among the
covariates will be examined by evaluating variance inflation factors. If collinearity is
present, only one of the correlated variables will be entered into the model at a time.
Analysis will be rerun choosing alternative correlated variables and the models will be
compared. The model with the lowest Akaike information criterion (AIC) will be chosen as the
final model. Model selection will include stepwise, forward selection, and backwards
elimination. The Hosmer-Lemeshow test will be used to determine goodness of fit.
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Observational Model: Case Control, Time Perspective: Prospective
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