BCG vaccination at birth and early childhood hospitalisation: a randomised clinical multicentre trial

Lone Graff Stensballe, Signe Sørup, Peter Aaby, Christine Stabell Benn, Gorm Greisen, Dorthe Lisbeth Jeppesen, Nina Marie Birk, Jesper Kjærgaard, Thomas Nørrelykke Nissen, Gitte Thybo Pihl, Lisbeth Marianne Thøstesen, Poul-Erik Kofoed, Ole Pryds, Henrik Ravn, Lone Graff Stensballe, Signe Sørup, Peter Aaby, Christine Stabell Benn, Gorm Greisen, Dorthe Lisbeth Jeppesen, Nina Marie Birk, Jesper Kjærgaard, Thomas Nørrelykke Nissen, Gitte Thybo Pihl, Lisbeth Marianne Thøstesen, Poul-Erik Kofoed, Ole Pryds, Henrik Ravn

Abstract

Background: The BCG vaccine is administered to protect against tuberculosis, but studies suggest there may also be non-specific beneficial effects upon the infant immune system, reducing early non-targeted infections and atopic diseases. The present randomised trial tested the hypothesis that BCG vaccination at birth would reduce early childhood hospitalisation in Denmark, a high-income setting.

Methods: Pregnant women planning to give birth at three Danish hospitals were invited to participate. After parental consent, newborn children were allocated to BCG or no intervention within 7 days of age. Randomisation was stratified by prematurity. The primary study outcome was number of all-cause hospitalisations analysed as repeated events. Hospitalisations were identified using The Danish National Patient Register. Data were analysed by Cox proportional hazards models in intention-to-treat and per-protocol analyses.

Results: 4184 pregnant women were randomised and their 4262 children allocated to BCG or no intervention. There was no difference in risk of hospitalisation up to 15 months of age; 2129 children randomised to BCG experienced 1047 hospitalisations with a mean of 0.49 hospitalisation per child compared with 1003 hospitalisations among 2133 control children (mean 0.47), resulting in a HR comparing BCG versus no BCG of 1.05 (95% CI 0.93 to 1.18) (intention-to-treat analysis). The effect of BCG was the same in children born at term (1.05 (0.92 to 1.18)) and prematurely (1.07 (0.63 to 1.81), p=0.94). The effect was also similar in the two sexes and across study sites. The results were essentially identical in the per-protocol analysis and after adjustment for baseline characteristics.

Conclusions: BCG vaccination at birth did not reduce the risk of hospitalisation for somatic acquired disease until 15 months of age in this Danish study population.

Trial registration number: NCT01694108, results.

Keywords: Bacillus Calmette-Guérin (BCG; hospitalisation; infant; non-specific effect; vaccine.

Conflict of interest statement

Competing interests: None declared.

Published by the BMJ Publishing Group Limited. For permission to use (where not already granted under a licence) please go to http://www.bmj.com/company/products-services/rights-and-licensing/.

Figures

Figure 1
Figure 1
Flow chart. Data collection of The Danish Calmette Study, by telephone interviews, clinical examinations and health registers. Percentages in parentheses (): Percentage among the eligible children. Percentages in square brackets []: Percentage among all randomised children. *Interviews conducted between child age 2–4 months: BCG 98.1% (2089/2129), control 96.8% (2064/2133). #Interviews conducted between child age 10–14 months: BCG 97.9% (2084/2129), control 96.2% (2052/2133).
Figure 2
Figure 2
Estimated mean number of all-cause hospitalisations per child for children randomised to BCG or no BCG.

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