Abstract
Background: Vitamin A supplementation significantly reduces all-cause mortality when given between 6-59 months of age, but has a null or detrimental effect when given between 1-5 months. Studies of neonatal vitamin A supplementation conducted across Africa and South Asia have produced conflicting findings. These age-pattern variations might result from immunological interactions between vitamin A supplementation and vaccines. Knowledge on the potential immunological sequelae of human neonatal vitamin A supplementation is so scarce that the foremost aim of this study is to seek indicative data on aspects of immunity likely to be affected by neonatal vitamin A supplementation. The objective of this trial is to test whether human neonatal vitamin A supplementation modulates immune function including improved thymic maturation in infancy and improved systemic immune responses to routine immunization.Methods/design: In an area of moderate vitamin A deficiency in a peri-urban area of The Gambia, 200 mother-infant pairs were enrolled in a double-blind randomised controlled trial. Within 48 hours of birth, neonates were randomised with stratification by birth weight and sex to receive either an oral dose of 50,000 IU vitamin A or placebo. Expanded Programme of Immunisation birth vaccinations were administered after supplementation, with subsequent vaccinations administered at 8, 12 and 16 weeks of age. A range of immunological outcomes were examined up to 17 weeks of age, with additional morbidity and anthropometry follow-up carried out throughout the first year of life. The primary endpoint of this trial is the frequency of circulating T regulatory (Treg) cells expressing gut homing receptors in infants at 17 week post-supplementation, with secondary outcomes including thymus maturation and B cell immune responses.Discussion: Indicative immunological data from this trial (and its Bangladeshi counterpart), will complement the larger randomised controlled trials (conducted in India, Tanzania and Ghana), on the effectiveness and safety of neonatal vitamin A supplementation in improving infant survival. Combined these trials, in addition to the existing trials, will inform policy.Trial registration: clinicaltrials.gov NCT01476358.
Original language | English |
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Article number | 92 |
Journal | BMC Pediatrics |
Volume | 14 |
Issue number | 1 |
DOIs | |
Publication status | Published - 4 Apr 2014 |
Externally published | Yes |
Bibliographical note
Funding Information:This trial is supported by the World HealthOrganization via Bill and Melinda Gates Foundation funding (2010/98441-0) and the Medical Research Council (UK), through core funding to the MRC International Nutrition Group (MC-A760-5QX00). This trial was sponsored by the London School of Hygiene and Tropical Medicine. Thanks to Dr Lisa Rogers and Dr Jaun Pablo Peña-Rosas, (Department of Nutrition for Health and Development, WHO) for technical support and coordination for the trials. Thanks to the Infant Immunology Laboratory (led by Dr Ed Clarke) and Vaccinology Theme (led by Prof Beate Kampmann), MRC Unit The Gambia, for operational support. We thank all trial staff, the staff based at MRC Sukuta field site and Sukuta Health Centre. We also acknowledge the support of the mothers and infants without whom this trial could not have taken place.
Keywords
- Africa
- Double blind randomised control trial
- Immune responses
- Neonatal
- Vitamin A supplementation