| Literature DB >> 30886409 |
Christian Pou1, Dieudonné Nkulikiyimfura1, Ewa Henckel2,3, Axel Olin1, Tadepally Lakshmikanth1, Jaromir Mikes1, Jun Wang1, Yang Chen1, Anna Karin Bernhardsson1,3, Anna Gustafsson2,3, Kajsa Bohlin2,3, Petter Brodin4,5.
Abstract
All circulating immunoglobulin G (IgG) antibodies in human newborns are of maternal origin1 and transferred across the placenta to provide passive immunity until newborn IgG production takes over 15 weeks after birth2. However, maternal IgG can also negatively interfere with newborn vaccine responses3. The concentration of IgG increases sharply during the third trimester of gestation and children delivered extremely preterm are believed to largely lack this passive immunity1,2,4. Antibodies to individual viruses have been reported5-12, but the global repertoire of maternal IgG, its variation in children, and the epitopes targeted are poorly understood. Here, we assess antibodies against 93,904 epitopes from 206 viruses in 32 preterm and 46 term mother-child dyads. We find that extremely preterm children receive comparable repertoires of IgG as term children, albeit at lower absolute concentrations and consequent shorter half-life. Neutralization of the clinically important respiratory syncytial virus (RS-virus) was also comparable until three months of age. These findings have implications for understanding infectious disease susceptibility, vaccine development, and vaccine scheduling in newborn children.Entities:
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Year: 2019 PMID: 30886409 DOI: 10.1038/s41591-019-0392-8
Source DB: PubMed Journal: Nat Med ISSN: 1078-8956 Impact factor: 53.440