Pregnancy IFN-γ responses to foetal alloantigens are altered by maternal allergy and gravidity status

During pregnancy, variations in maternal-foetal cellular interactions may influence immune programming. This study was carried out to determine if maternal responses to foetal alloantigens are altered by maternal allergic disease and/or previous pregnancies. For this cohort study, peripheral blood w...

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Veröffentlicht in:Allergy 2008-11, Vol.63 (11), p.1473-1480
Hauptverfasser: Breckler, L.A, Hale, J, Taylor, A, Dunstan, J.A, Thornton, C.A, Prescott, S.L
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Sprache:eng
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Zusammenfassung:During pregnancy, variations in maternal-foetal cellular interactions may influence immune programming. This study was carried out to determine if maternal responses to foetal alloantigens are altered by maternal allergic disease and/or previous pregnancies. For this cohort study, peripheral blood was collected from allergic (n = 69) and nonallergic (n = 63) pregnant women at 20, 30, 36-week gestation and 6-week postpartum (pp). Cord blood was collected at delivery. Mixed lymphocyte reactions were used to measure maternal cytokine responses [interleukin-6 (IL-6), IL-10, IL-13 and (interferon-γ) IFN-γ] at each time point towards foetal mononuclear cells. Maternal cytokine responses during pregnancy (20, 30 and 36 weeks) were suppressed compared to the responses at 6-week pp. The ratio of maternal IFN-γ/IL-13 and IFN-γ/IL-10 responses were lower during pregnancy. Allergic mothers had lower IFN-γ responses at each time-point during pregnancy with the greatest difference in responses observed at 36-week gestation. When allergic and nonallergic women were further stratified by gravidity group, IFN-γ responses of allergic multigravid mothers were significantly lower than nonallergic multigravid mothers during pregnancy. During normal pregnancy, peripheral T-cell cytokine responses to foetal alloantigens may be altered by both allergic status of the mother and previous pregnancies. These factors could influence the cytokine milieu experienced by the foetus and will be further explored in the development of allergic disease during early life.
ISSN:0105-4538
1398-9995
0108-1675
DOI:10.1111/j.1398-9995.2008.01718.x