Perinatal colonization with S. aureus may trigger the occurrence of sCD14 in plasma, which may influence development of the infantile immune system and risk of allergy development.
BackgroundThe role of FOXP3+ regulatory T cells in the prevention against sensitization
and allergy development is controversial.ObjectiveWe followed 65 newborn Swedish children from farming and non-farming families from birth to
3 years of age and investigated the relation between CD4+ T cell subsets in
blood samples and development of sensitization and allergic disease.MethodsThe proportions of FOXP3+CD25high,
CTLA-4+CD25+, CD45RO+,
HLA-DR+, CCR4+ or α4β7+ within
the CD4+ T cell population were examined by flow cytometry of blood samples at
several time-points. Mononuclear cells were isolated from blood and stimulated with birch allergen,
ovalbumin or the mitogen PHA, and the levels of IL-1β, IL-6, TNF, IFN-γ, IL-5 and
IL-13 were measured. A clinical evaluation regarding the presence of allergen-specific IgE and
allergy was performed at 18 and 36 months of age.ResultsMultivariate discriminant analysis revealed that children who were sensitized at 18 or
36 months of age had higher proportions of FOXP3+CD25high T
cells at birth and at 3 days of life than children who remained non-sensitized, whereas
allergy was unrelated to the neonatal proportions of these cells. The proportions of
CTLA-4+CD25+ T cells were unrelated to both sensitization and
allergy. The association between higher proportions of FOXP3+CD25high T
cells and sensitization persisted after exclusion of farmer's children. Finally, a farming
environment was associated with lower proportions of FOXP3+CD25high T
cells in early infancy and to a more prominent T cell memory conversion and cytokine production.Conclusion & Clinical RelevanceOur results indicate that high proportions of FOXP3+CD25high T cells
in neonates are not protective against later sensitization or development of allergy.
Early intestinal colonization by toxigenic S. aureus strains seems to promote systemic IgA responses. Furthermore, high levels of APRIL and IgA in the circulation at 4 months of age seem to correlate negatively with allergy development.
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