Time of perinatal immunization, thimerosal exposure and neurodevelopment at 6 months in breastfed infants

Aim: Brazilian newborns immunized with hepatitis‐B (thimerosal containing vaccine, TCV) receive the first dose within 24 h if delivered in public hospitals, but at a later time if born in private hospitals. We compared neurodevelopment (ND) in infants born in a state hospital (immunized within 24 h)...

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Bibliographic Details
Published in:Acta Paediatrica 2007-06, Vol.96 (6), p.864-868
Main Authors: Marques, Rejane C, Dórea, José G, Manzatto, Angelo G, Bastos, Wanderley R, Bernardi, José VE, Malm, Olaf
Format: Article
Language:English
Subjects:
Biological and medical sciences
Body Weight
Brazil
Breast Feeding
Breastfeeding
Developmental Disabilities - chemically induced
Ethylmercury
Ethylmercury Compounds - administration & dosage
Ethylmercury Compounds - adverse effects
Female
General aspects
Hepatitis B Vaccines - administration & dosage
Hepatitis B Vaccines - chemistry
Humans
Immunization Schedule
Infant, Newborn
Male
Maximum Tolerated Dose
Medical sciences
Neurodevelopment
Neuropsychological Tests
Preservatives, Pharmaceutical - administration & dosage
Preservatives, Pharmaceutical - adverse effects
Prevention and actions
Public health. Hygiene
Public health. Hygiene-occupational medicine
Thimerosal
Thimerosal - administration & dosage
Thimerosal - adverse effects
Time Factors
Vaccines
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Summary:Aim: Brazilian newborns immunized with hepatitis‐B (thimerosal containing vaccine, TCV) receive the first dose within 24 h if delivered in public hospitals, but at a later time if born in private hospitals. We compared neurodevelopment (ND) in infants born in a state hospital (immunized within 24 h) and in privately run hospitals (immunized 2–4 days postnatally). Methods: We used the Gesell Developmental Schedules in 82 healthy exclusively breastfed infants at 6 months to assess motor skills, language development, comprehension capacity and social skills. Results: Compared to the group immunized 2–4 days after hospital discharge, the group immunized within 24 h showed no significant difference in ND delays. Despite the variation in gestational age (range 36–42 weeks) and TCV‐ethylmercury (EtHg) dose (5.7–11.3 μgHg/kg b.w.) at birth, time of exposure to TCV showed no significant association with ND. Gesell Developmental Score was not significantly correlated with total parenteral EtHg/unit of body mass neither with the relative increase in hair‐Hg (as an additional challenge to prenatal Hg exposure). Conclusion: In breastfed infants, differences in early exposure to TCV‐EtHg cannot portend clinical neurodevelopment delays at 6 months. We speculate that breastfeeding remains a significant strategy to improve central nervous system protection of infants facing early exposure challenges.
ISSN:0803-5253
1651-2227
DOI:10.1111/j.1651-2227.2007.00288.x