Diarrhoea Clinical Trial
Official title:
An Observational Study to Evaluate Causes of Rotavirus Vaccine Failure in Zambian Children in the Context of Routine Immunization Services
Verified date | July 2018 |
Source | Centre for Infectious Disease Research in Zambia |
Contact | n/a |
Is FDA regulated | No |
Health authority | |
Study type | Observational |
Zambia recently introduced routine infant immunization against rotavirus - the most important
cause of severe gastroenteritis and diarrhoea mortality in children. Although vaccines like
Rotarix are a cost effective tool against infectious diseases, live oral vaccines can be less
immunogenic and efficacious in developing world settings as compared with industrialized
countries. Reasons behind this phenomenon are not well understood, but may relate to
continued maternal antigen exposure and high level maternal immunity that is passed to the
foetus/newborn transplacentally and/or through breast milk.
Therefore, three arising hypotheses include: (i) high-level rotavirus-specific maternal
immunity (in the form of anti-rotavirus breast-milk immunoglobulin A (IgA) and transplacental
serum IgG) is a major contributor to failed seroconversion following infant vaccination. (ii)
Malnutrition negatively impacts infant immunity and increases the risk of post-vaccination
rotavirus gastroenteritis. (iii) Introduction of rotavirus vaccine will alter the molecular
epidemiology of circulating rotavirus strains detected in vaccinated children presenting with
severe diarrhea.
To address these hypotheses, the proposed study will recruit a prospective cohort of 420
mother-infant pairs. These will be enrolled at the time of vaccination and followed for up to
four years. Baseline immunological status will be ascertained and seroconversion rates
determined a month after full immunization. Incident rotavirus gastroenteritis will be
monitored in the vaccinated infants whenever episodes of diarrhoea occur; through this
surveillance, the sero-strains of rotaviruses causing disease will be tracked over the four
year period. Contributions of HIV infection both in mothers and infants, vitamin A and zinc
deficiency, weight for age Z-scores as well as mid upper arm circumference will also be
assessed. Knowledge gained from this study will inform future interventional trials on
strategies to improve rotavirus vaccine effectiveness in the developing world.
Status | Completed |
Enrollment | 420 |
Est. completion date | April 30, 2016 |
Est. primary completion date | April 30, 2015 |
Accepts healthy volunteers | Accepts Healthy Volunteers |
Gender | All |
Age group | 6 Weeks to 15 Weeks |
Eligibility |
Inclusion Criteria: - Mother willing to participate voluntarily and able to provide signed informed consent (with witness in the case of illiterate participant) - Infant eligible for rotavirus vaccine immunization as per national policy (male or female infant, 6-12 weeks old) - Mother willing to undergo study procedures, including questionnaires, HIV counselling and testing, CD4 testing, and provide breast milk and blood sample at enrolment. - Mother willing for child to undergo study procedures including full-course rotavirus vaccination, phlebotomy at enrolment and 1 month post-rotavirus vaccination, and presentation to clinic for collection of stool sample when infant has diarrhoea. - Plans to remain resident in the area and willing to come for scheduled visits for the duration of the study. Exclusion Criteria: - Contraindication to rotavirus vaccination. - Previous administration of rotavirus vaccine to child. - Recent immunosuppressive therapy in child (including high-dose systemic corticosteroids). - History of ever receiving a blood transfusion or blood products, including immunoglobulins within the last 6 months, for mother and child. - Mother plans for herself or child to move away from the study catchment area within the next two years. - Any condition deemed by the study investigator to pose potential harm to the participants or jeopardize the validity of study results. |
Country | Name | City | State |
---|---|---|---|
Zambia | Centre for Infectious Disease Research in Zambia | Lusaka |
Lead Sponsor | Collaborator |
---|---|
Centre for Infectious Disease Research in Zambia | National Institute of Allergy and Infectious Diseases (NIAID) |
Zambia,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Other | Sero-epidemiology of Breakthrough Rotavirus Infection in Immunized Infants | Determination of genotype in every rotavirus causing severe gastroenteritis will be done each time stool samples are collected for diarrhoea. Patients presenting with any diarrhoea will be tested for rotavirus and staged clinically (by Vesikari score). Those with severe disease (e.g., Vesikari >11/20) will be processed for genotype. Thus, we will identify the number of rotavirus cases following vaccination as well as identify the strain in those with severe disease. This will allow for "wild type versus vaccine"strain mismatch evaluation. We anticipate that the circulating strains in the community will change in response to vaccine pressure at the population level. However, when interpreting reasons for vaccine failure, it is critically important to evaluate strain mismatch because the way to approach this type of breakthrough disease is dramatically different than if there is breakthrough infection to vaccine strain rotavirus. |
42 months | |
Primary | Proportion of Immunized Infants Exposed to High Breast Milk Anti-rotavirus Immunoglobulin-A Who Fail to Seroconvert | The primary exposure in this cohort is maternal IgA status, as we believe breast milk IgA is the most critical factor in failed vaccination, and maternal IgA has previously been estimated to be either high level (approximately 55%) or undetectable or low level (approximately 45%). We will collect maternal serum and breast-milk IgA at the time of vaccination and then measure infant anti-rotavirus-specific serum IgA levels 1 month following the second dose of Rotarix™ (GlaxoSmithKline) rotavirus vaccine. |
1 month following full immunization | |
Primary | Proportion of Immunized Infants Exposed to Transplacentally-acquired, Rotavirus-specific, Infant Serum IgG Who Fail to Sero-convert. | The co-primary exposure in this cohort is transplacentally acquired anti-rotavirus immunoglobulin-G. We will collect infant serum at baseline before any vaccination and then measure the levels of anti-rotavirus-specific serum IgG and will also obtain the same at 1 month following the second dose of Rotarix™ rotavirus vaccine. |
1 month after full immunisation | |
Primary | Proportion of Immunized Infants Exposed to Maternal HIV Infection Who Fail to Seroconvert | To evaluate whether maternal HIV infection (as well as level of CD4 count) affects infant vaccine take, we will collect the maternal HIV status, (and CD4 count if +ve). We will then correlate the maternal HIC status and CD4 count levels to infant zero conversion at 1 month after the two vaccine doses. | 1 month after the two vaccine doses | |
Secondary | Proportion of Immunized Infants With Low Micronutrient Levels (as Indicated by Serum Zinc and Vitamin A), Who Fail to Seroconvert | To evaluation whether nutritional status affects vaccine take, we will assess the immunized infant's nutritional status as indicated by serum level of zinc and vitamin A. These will be correlated to seroconversion results. | 1 month after full immunization |
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