Rotavirus Gastroenteritis Clinical Trial
Official title:
Introduction of an Oral Live Human Rotavirus (Rotarix) Vaccine in Matlab
The study will be conducted in the Matlab Health and Demographic Surveillance System (HDSS)
field area of the International Centre for Diarrhoeal Disease Research, Bangladesh (ICDDR,B)
to determine the population effectiveness of Rotarix in Bangladeshi children. Villages in
both intervention and government comparison areas will be included in this evaluation. We
propose to introduce Rotarix into half of the villages of the Matlab HDSS. In villages
randomized to receive the vaccine, all eligible children will be offered Rotarix during
their first two Expanded Programme on Immunization (EPI) visits, as would routinely be done
if Rotarix were included in the Government EPI schedule. In villages randomized not to
receive Rotarix, children will receive their EPI vaccinations exactly as they would have in
the absence of this study. Administration of Rotarix will be conducted by regular EPI staff,
but ICDDR,B study staff will be present to document informed consent and collect
study-specific information. The Ministry of Health will be an active partner in this
evaluation since they will be the agency which may follow up with any subsequent vaccine
programme. Vaccination with Rotarix will be recorded on the infant's immunization card which
is normally used by the EPI programme, but also on a separate study-specific data collection
form.
Vaccination with Rotarix will continue from study initiation through June 30, 2011.
Surveillance for rotavirus gastroenteritis will occur at Matlab Diarrhoeal Hospital and the
community treatment centres of the Matlab HDSS continuously throughout the study period.
Diarrheal illness information collected through surveillance will be linked to Rotarix
study-specific data through the subject's HDSS identification numbers. The primary study
endpoint will be the occurrence of an illness episode of acute diarrhoea, among infants and
children admitted to a medical facility, determined to be caused by wild-type rotavirus
found in a stool specimen. At the end of the surveillance period, rates of this primary
study endpoint among age-eligible infants will be compared for villages randomized to
receive Rotarix versus for villages randomized not to receive Rotarix. We expect that the
rates of rotavirus diarrhoea will be significantly lower among children from the vaccinated
villages.
The first participant was enrolled in the study on September 23, 2008. Till date (May 12,
2010) a total of 2,882 participants have been enrolled and received first dose. 2,684
participants received second dose of Rotarix. There were 1013 cases gastroentritis reported
to diarrhoeal treatment centres among <2 years old children from the vaccinated and
unvaccinated villages. There were six death cases among the children who received Rotarix
vaccine. These death cases were not related to the vaccines/study products.
This trial will determine the population effectiveness of Rotarix in Bangladeshi infants.
The study will be conducted in both the government comparison area and the intervention area
of the Matlab HDSS. To carry out the evaluation, we will introduce the Rotarix vaccine into
half of the villages of the HDSS area. In villages randomized to receive Rotarix, the study
will be explained to parents and if they consent to their child's participation and the
child is eligible, the child will receive two doses of Rotarix during their first two EPI
visits (scheduled for 6 and 10 weeks of age), if possible, as would routinely be done if
Rotarix were included in the government programme. Administration of Rotarix will be
conducted by regular EPI staff, but ICDDR,B study staff will be present to document informed
consent and collect study-specific information. Vaccination with Rotarix will be recorded on
the infant's immunization card which is normally used by the EPI programme, but also on a
separate study-specific data collection form. Participation in the study will not affect a
subject's receipt of other routine childhood immunizations or other medical care. In
villages randomized not to receive Rotarix, children will receive their EPI vaccinations
exactly as they would have in the absence of this study.
Surveillance for will be conducted at the Matlab Diarrhoeal Hospital and the two community
treatment centres at Nayergaon and Kalirbazaar, which facilitate quick and easy
accessibility of treatment for life-threatening diarrhoeal diseases from the HDSS area. The
main study outcome will be episodes of rotavirus diarrhoea among children admitted to Matlab
Diarrhoeal Hospital or either of the two community treatment centres (Nayergaon and
Kalirbazaar). Study personnel will record the child's symptoms and clinical history, and
collect a fecal specimen for laboratory testing for rotavirus. The identity of the child
will be confirmed through the HDSS subject identification number system. All patients coming
to the Matlab Diarrhoea Hospital and Nayergoan community treatment centre from these
villages are already included in the Matlab diarrhoea surveillance system, and faecal
samples are routinely tested for rotavirus and other pathogens, with results linked to
demographic and health databases of the HDSS. Kalirbazaar treatment centre is not currently
included in the current surveillance system, but we will establish surveillance at this
centre during this study. For enrolled participants who present to one of the treatment
facilities, illness information and test results will be linked to HDSS demographic data and
study-specific data collected at enrolment through the subject's HDSS number. For residents
not enrolled who present to a treatment facility, illness information will be linked only to
HDSS demographic data, as is already being done as part of surveillance activities.
Rates of acute gastroenteritis caused by rotavirus and other agents among age-eligible
infants will be compared for infants (vaccinated and unvaccinated) from villages randomized
to receive Rotarix versus for those (unvaccinated) from villages randomized not to receive
Rotarix. We expect that the rates of diarrhoea will be significantly lower among children
from the vaccinated villages, but that rates of diarrhoea caused by other pathogens may be
similar. (This second analysis - a "control analysis" - will be helpful to verify a lack of
bias in health seeking behaviours since one would expect that cholera, ETEC, Salmonella and
Shigella gastroenteritis rates would be similar in the two groups.). These cases will be
detected from all patients of all ages who come to the Matlab Diarrhoeal Hospital or the
community treatment centres (Nayergaon or Kalirbazaar), but the primary analysis will
include only those rotavirus diarrhoea cases among children who had been age-eligible for
vaccination in their respective villages.
Although not a blinded evaluation, the introduction of bias will be reduced in several ways.
First, the vaccine teams located in the EPI centres that are completely separate from the
clinical settings where clinicians will be conducting surveillance. Second, the clinicians
are separated from those scientists conducting laboratory testing. Third, laboratory assays
for rotavirus will be carried out in the laboratory in Dhaka using coded specimens and are
not conducted at the time of illness (since they have little clinical value). Although a
parent could inform the clinician as to his/her child's participation in the study, this is
believed to be an unlikely or important source of bias for two reasons. One, most rotavirus
gastroenteritis is not seen until later than 6 months after an infant's second dose of
Rotarix, and there will be no active follow-up among parents after last receipt of Rotarix.
Thus, there is a reduced likelihood that parents will remember that their child had received
a vaccination targeted specifically against one type of severe diarrhoea. Second, Matlab
Diarrhoeal Hospital and the community treatment centres have been caring for severe
diarrhoea for many years and the entire community is already accustomed to attending the
facilities for such illnesses. Thus, there is a reduced likelihood parents of vaccinated and
unvaccinated infants are going to have differential diarrhoeal illness treatment-seeking
behaviors.
Again, the study will be conducted in both the government comparison area and the
intervention area of Matlab HDSS. Enrolment will begin in the government comparison area no
later than June 1, 2008. Enrolment will begin in the intervention area January 1, 2009.
Surveillance for rotavirus diarrhoea will occur continuously and concurrently to enrolment
activities. Enrolment in both areas will cease on June 30, 2010, but surveillance for
rotavirus gastroenteritis will occur until December 31, 2010.
By in January 1, 2009, it is expected that less than 15% of children less than 2 years of
age in the intervention area will have received Rotateq in the Merck trial. Nonetheless, we
will stratify randomization within the intervention area by rates of participation in that
trial for each village. Additionally, because we will have the full dataset for Matlab for
the Rotateq trial, we will be able to analyze any impact of that Rotateq trial on the
Rotarix evaluation within the intervention area.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Prevention
Status | Clinical Trial | Phase | |
---|---|---|---|
Completed |
NCT01575197 -
Evaluation of the Human Rotavirus Vaccine at Varying Schedules and Doses in Rural Ghana
|
Phase 4 | |
Completed |
NCT01202201 -
A Retrospective Survey of the Burden of Rotavirus Gastroenteritis (RV GE) and Nosocomial RV GE in Japan
|
N/A | |
Completed |
NCT00953056 -
A Study of V260 in Healthy Chinese Adults, Children and Infants (V260-028)(COMPLETED)
|
Phase 1 | |
Completed |
NCT04185545 -
Efficacy, Safety and Immunogenicity of Rotavirus RV3 Vaccine (Bio Farma) in Neonates
|
Phase 3 | |
Completed |
NCT03474055 -
Study on Liquid Bovine Rotavirus Pentavalent Vaccine (LBRV-PV) to Evaluate Lot-to-Lot Consistency and to Compare Non-Inferiority With ROTASIIL (Lyophilized BRV-PV) in Healthy Infants in India
|
Phase 2/Phase 3 | |
Completed |
NCT01236066 -
Impact of Rotavirus Vaccination on Hospitalisations for Rotavirus Gastroenteritis in Children Aged <5 Years in Australia
|
N/A | |
Completed |
NCT00489567 -
Hospital-based Surveillance to Collect Prospective Data to Estimate the Disease Burden of Severe RV GE in Sweden
|
N/A | |
Completed |
NCT02584816 -
Phase III Study on Rotavirus Vaccine to Evaluate Lot-to-lot Consistency and Interference With Routine UIP Immunization
|
Phase 3 | |
Completed |
NCT02062385 -
Efficacy, Safety, and Immunogenicity of V260 in Healthy Chinese Infants (V260-024)
|
Phase 3 | |
Completed |
NCT02133690 -
A Clinical Trial to Study the Effect and Safety of Rotavirus Vaccine Against Severe Rotavirus Gastroenteritis in Healthy Indian Infants
|
Phase 3 | |
Completed |
NCT01177657 -
Study to Evaluate the Effectiveness of Rotarix™ Against Severe Gastroenteritis Among Hospitalized Children in Brazil
|
N/A | |
Completed |
NCT00740935 -
Impact of Systematic Infants Vaccination Against Rotavirus on Gastroenteritis Hospitalization: a Prospective Study in Brest District, France.
|
Phase 4 | |
Completed |
NCT01265355 -
Community Based Prevention of Rotavirus Gastroenteritis by a Functional Food Supplement
|
Phase 2/Phase 3 | |
Completed |
NCT00169455 -
Assess the Immunogenicity of the Human Rotavirus (HRV) Vaccine After Reconstitution Without Buffering Agent; & Evaluate the Immunogenicity, Reactogenicity & Safety of the Vaccine After Storage for 7 d at 37°C Following 2 Doses in Healthy Infants
|
Phase 3 | |
Completed |
NCT04819412 -
To Determine the Safety and Efficacy of Liquid ROTAVAC 5C Vaccine Against Childhood Diarrhea Caused by Rotavirus
|
Phase 3 | |
Completed |
NCT02728869 -
Safety, Reactogenicity and Immunogenicity of Heat-stable Rotavirus Vaccine (HSRV) in Adults and Infants
|
Phase 1/Phase 2 | |
Recruiting |
NCT05958771 -
The Efficacy of Three Doses of Live Attenuated, Oral Rotavirus Vaccine 116E
|
Phase 3 | |
Recruiting |
NCT01061658 -
Safety and Immunogenicity Study of the Tetravalent Rotavirus Vaccine
|
Phase 1/Phase 2 | |
Completed |
NCT01508533 -
Epidemiology of Rotavirus Infection in North India Community
|
N/A | |
Completed |
NCT01026779 -
Rotavirus Gastroenteritis and Vaccine Usage in Rhode Island
|