Tuberculosis Clinical Trial
Official title:
BCG Vaccination and Childhood Morbidity and Mortality: Interventions With Possible Implications for the Immunisation Policy in Developing Countries. Should Low Birth Weight Infants Be Vaccinated With BCG Vaccine at Birth?
The World Health Organization (WHO) currently recommends BCG vaccination at birth in developing countries. Pre-term infants should be vaccinated when they reach the chronological age of 40 weeks. Due to difficulties in establishing the correct gestational age, the vaccination policy for BCG in many developing countries is defined by birth weight rather than by gestational maturity. In the study area, low birth weight (LBW) infants (< 2500 g) are not supposed to be vaccinated at birth; instead the mother is asked to return for vaccination when the child has gained sufficient weight. BCG has marked immune stimulatory effects in both animal and human studies and observational studies suggest that BCG is associated with a non-specific reduction in mortality in areas with high infant and child mortality. The specific objective of the study is to examine the effect of early vaccination of LBW children for adverse events, purified protein derivative of tuberculin (PPD) reaction, scar size, morbidity, and mortality in a randomised prospective study of BCG vaccination at birth versus later (according to policy) among children 19 months of age in Guinea-Bissau. The hypothesis is that BCG vaccination of low birth weight (LBW) children at birth reduces infant mortality of this high-risk group by 25%.
Criteria for verification: 1,600 low birth weight (LBW) infants recruited at the national
hospital and local health centres and enrolled in a randomised trial of BCG vaccination at
birth versus later vaccination; information on potential adverse events following early BCG
vaccination of LBW infants; follow-up of children to 12 months of age with home visits at 2,
6 and 12 months of age; assessment of tuberculin reaction and scar-formation at 2, 6 and 12
months of age; assessment of BCG vaccination coverage during infancy; and assessment of
all-cause mortality during infancy.
Recruitment: All LBW children delivered at the maternity ward of the national hospital at
the local Health Centre will be offered enrolment in the study. Furthermore, all children
born at home in the study area will be weighed and referred for BCG vaccination at the
health centres as quickly as possible. For mothers of LBW children, the current policy and
the purpose of the study will be explained. If she accepts participation, she will draw a
randomisation number indicating whether the children will be BCG vaccinated early or not. At
the time of enrolment, children will be examined clinically with anthropometrics, and major
risk factors will be documented (including TB exposure at home, recent infections, access to
malaria drugs, ethnic group, schooling, housing conditions, mother's recent drug
consumption). Newborns will only be included in the study if they are considered
sufficiently healthy to be discharged from the hospital, or when they arrive at the health
centre if born at home. Twins will be a large part of the LBW children as twinning is common
in the study area (around 2% of births). They will be allocated to the same group, as there
could be confusion for the mother as to who had been vaccinated. As is happening at the
moment, mothers of children not receiving vaccination at birth will be recommended to attend
a local health centre as soon as the child has gained weight. For ethical reasons, it will
not be possible to use a placebo as this could mean that some children would not be BCG
vaccinated if the mother believed that the child had in fact been vaccinated. The children
who are not vaccinated initially will subsequently be vaccinated at the limited number of
health centres in the capital, which administer BCG vaccination. The intradermal vaccination
technique and vaccine storage will be supervised, and it will be monitored as to whether
scar-formation and PPD reactivity is similar in children vaccinated at the different centres
to assure that vaccinations have been administered in the same way.
Follow-up: To assure proper identification of the children, the mother and newborn child
will be driven home to document the location of the home. The children included in the study
will be visited at 2, 6, and 12 months of age, to identify subsequent BCG vaccinations by
inspection of the vaccination card, to weigh the child and measure arm-circumference, to
assess BCG scarring and to document morbidity, hospitalisations and survival. Sick children
identified during these visits will be referred for treatment at the relevant health
institution. If the child has still not been vaccinated, the mother will be encouraged to
bring the child for vaccination. Should the child have died, a verbal autopsy will be
conducted. The children will be followed for morbidity, hospitalisations, and mortality up
to 12 months of age. Within the study area they may be followed longer. In order to assure
detection of possible complications to BCG vaccination, LBW children enrolled in the study
will be provided with a card identifying the child, and the mother will be told to bring the
child for consultation at the local Health Centre where consultations and treatment will be
free of charge. The expected very rare complications will be treated according to WHO's
recommendations.
A subgroup of the children will be enrolled in immunological studies. To assess the effect
of BCG vaccination on the immune profile, initially unvaccinated LBW children will have a
blood sample collected when they turn up for BCG vaccination at a health centre. For each
child examined, a BCG vaccinated LBW child matched for age and sex will be examined and a
blood sample collected.
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Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Prevention
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