BCG Revaccination With the Third Dose of Diphtheria-tetanus-pertussis Vaccine and Infant Mortality in Africa (BCG2-DTP3)

Background:

Since the 1970s, the basic vaccination schedule in low-income countries has sequenced BCG and DTP, so that BCG was provided at birth and diphtheria-tetanus-pertussis vaccine (DTP, now in a version with H. influenza vaccine and hepatitis B, 'pentavalent vaccine') in 3 doses at 6,10, and 14 weeks, followed by measles vaccine (MV) at 9 months of age.

WHO recommends DTP-after-BCG but a meta-analysis of observational studies has shown that co-administration of BCG+DTP is associated with 43% (27-54%) lower mortality than DTP after BCG (Higgins et al, BMJ 2016).

The idea that vaccines can change morbidity and mortality in ways not explained by prevention of the vaccine-targeted infection is gaining increasing recognition. Major examples of beneficial NSEs include that the live BCG vaccine reduces non-tuberculosis infections. In contrast, the non-live DTP vaccine is associated with increased susceptibility to non-DTP infections and higher female mortality.

When WHO reviewed the NSEs of vaccines, the DTP vaccine was associated with a 38% (-8-108%) increase in mortality, but providing BCG-with-DTP was associated with 48% (30-66%) lower mortality than the usual schedule of BCG-then-DTP.

Based on this evidence, the investigators propose an randomised controlled trial (RCT) to test whether co-administration of a second dose of BCG (BCG2) with the third dose of DTP (DTP3) reduces the severe morbidity rate and the F/M HR.

Hypotheses:

• BCG2+DTP3 vs. DTP3 reduces severe morbidity, i.e. non-accidental deaths and hospital admissions, by 25% until MV is given.
• BCG2+DTP3 vs. DTP3 reduces the F/M severe morbidity hazard ratio until MV is given.

Methods:

The RCT will be nested within the Bandim Health Project (BHP) Health and Demographic Surveillance System (HDSS) study area. The RCT will be conducted in the urban areas of the BHP HDSS, which follows approximately 100,000 inhabitants (www.bandim.org). The BHP registers pregnancies, births, and follow young children until 3 years of age. During home visits, data is collected regarding infections, hospitalisations, vaccinations, breastfeeding, growth, and survival. At the first contact, BHP assistants provide a vaccination card for the child, which serves as an ID card during subsequent health system contacts. At the home visits, mothers are encouraged to bring their children for vaccination. All vaccinations and consultations at the three health centres in the study area are documented. Furthermore, BHP registers deliveries and paediatric consultations and admissions at the Simão Mendes national hospital.

When the child is approaching 14 weeks of age, written (Portuguese) and verbal (Creole Portuguese) information will be provided during a home visit. Children, who are not seriously ill and whose parents are willing to take part, will be invited to the health centre for enrolment (see exclusion/inclusion criteria below).

At the centre, participants will be asked to obtain oral and written consent. It will be explained that the Ministry of Health does not routinely recommend BCG2. However, studies from several countries suggest that BCG can improve health. Therefore, it will be examined whether the addition of BCG2 contributes to better child health. Those who wish to take part in the study are asked to sign consent forms (or in case of illiteracy provide thumb print on consent forms).

The child's vaccination card will be transcribed, and the child will be examined by a clinician. Both mother and child will be examined for BCG-scars. Finally, the children will be randomised to BCG or no intervention (1:1 in blocks, stratified by sex, to BCG or no intervention with DTP3 using REDCap).

The investigators will not record BCG2/no intervention on the child's vaccination card, and all field assistants and hospital workers collecting outcome data will be unaware of the child's allocation. The mothers/guardians of participating children will know whether the child received BCG or No Intervention.

Enrolled children will be called every 2 months to assess vital status, hospitalizations and consultations. In case telephone contact is not achieved, a home visit will be conducted. At 9 months of age all children will be visited at home and invited to the health centre for clinical assessment.

Deaths are detected at the regular contacts. Within 3 months after a death, the family will be interviewed to conduct a verbal autopsy (VA). The cause of death will be based on the physician diagnosis for in-hospital deaths or the VA-history for children that died elsewhere. Based on this information, deaths will be classified as accidental or non-accidental.

Most admissions occur at the national paediatric ward and will be registered there by the BHP staff. At the regular contacts, the mother will be asked whether the child has been hospitalised. A questionnaire is completed for each admission to obtain timing, symptoms, duration, and place of admission. Admissions will be counted as non-accidental if the paediatric ward data indicates that it was not caused by an accident.

With a mortality risk of 1.5% and a hospitalisation risk of 7.5% between 14 weeks and 9 months, the study can detect a 25% reduction in deaths and hospitalisations with 4700 participants (power 80%; significance 5%). With a 9% risk of the composite outcome, there will be have considerable power to detect minor changes in the F/M severe morbidity ratio. Over 4-5 years of enrolment, the plan is to recruit 6000 children, allowing for loss to follow-up and potential interference from national campaigns.

Statistical analyses:

Cox regression models will be used to compare severe morbidity for BCG2+DTP3 versus controls (No intervention+DTP3). Children are followed from enrolment until death, migration, measles vaccination, age 12 months, or end of study. Potential effect modifiers will be investigated. Since vaccines interact, follow-up in the main analysis will be censored at vaccination campaigns and this could reduce the power of the study. However, OPV is the only vaccine used in campaigns in this age group and these campaigns are now rare.

All comparisons of BCG2+DTP3 vs No intervention+DTP3 will be analysed separately by sex. Potential effect modifiers besides sex include season, vaccination campaigns, BCG status, and BCG scar status of mother and child prior to enrolment.