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孕期过敏和非过敏母亲体内和体外细胞因子产生的调节。

Modulation of in vivo and in vitro cytokine production over the course of pregnancy in allergic and non-allergic mothers.

机构信息

School of Paediatrics and Child Health, University of Western Australia, Perth, WA, Australia.

出版信息

Pediatr Allergy Immunol. 2010 Feb;21(1 Pt 1):14-21. doi: 10.1111/j.1399-3038.2009.00880.x. Epub 2009 Mar 23.

DOI:10.1111/j.1399-3038.2009.00880.x
PMID:19490478
Abstract

Cytokines secreted during pregnancy may influence immune development of the foetus. This study aimed to determine if maternal allergy alters patterns of systemic cytokine production throughout and after pregnancy. Maternal plasma cytokines and allergen-specific production of interleukin (IL)-10, IL-13 and interferon (IFN)-gamma were measured in allergic (n = 63) and non-allergic (n = 70) pregnant women who had a full set of sequential peripheral blood samples collected at 20-, 30-, 36-wk gestation and 6-wk post-partum. Maternal allergy was strictly defined by both allergen sensitization and doctor-diagnosed asthma, eczema or rhinitis. IL-13 responses to allergen were higher for allergic mothers at all time-points (20 wk: p < 0.001; 30 wk: p = 0.001; 36 wk: p < 0.001; post-partum: p < 0.001). For the non-allergic group, IL-13 levels to house dust mite decreased from 20- to 36-wk gestation (Friedman ANOVA p = 0.012) and were significantly lower at 36 wk compared with post-partum (p = 0.002). In contrast, IL-13 production by allergic mothers did not change from 20 wk through to post-partum. For both allergic and non-allergic mothers, in vitro IFN-gamma production was lower at all pregnancy time-points compared with post-partum levels. Allergic women had an increased propensity for peripheral blood allergen-specific T helper-2 responses during pregnancy, and failed to downregulate these responses in comparison with non-allergic women. This may be a factor that contributes to the increased risk of atopy in infants born to allergic mothers.

摘要

怀孕期间分泌的细胞因子可能会影响胎儿的免疫发育。本研究旨在确定母体过敏是否会改变整个孕期和产后全身细胞因子产生的模式。在有完整的一系列外周血样本的过敏(n = 63)和非过敏(n = 70)孕妇中,测量了母体血浆细胞因子和白细胞介素(IL)-10、IL-13 和干扰素(IFN)-γ的过敏原特异性产生,这些孕妇在 20 周、30 周、36 周妊娠和产后 6 周时采集了全套外周血样本。母体过敏通过过敏原致敏和医生诊断的哮喘、湿疹或鼻炎严格定义。在所有时间点,过敏母亲对过敏原的 IL-13 反应均更高(20 周:p < 0.001;30 周:p = 0.001;36 周:p < 0.001;产后:p < 0.001)。对于非过敏组,对屋尘螨的 IL-13 水平从 20 周到 36 周妊娠下降(Friedman ANOVA p = 0.012),并且在 36 周与产后相比显著降低(p = 0.002)。相比之下,过敏母亲的 IL-13 产生从 20 周到产后都没有变化。对于过敏和非过敏的母亲,与产后水平相比,所有妊娠时间点的体外 IFN-γ产生均较低。在怀孕期间,过敏女性对外周血过敏原特异性辅助性 T 细胞 2 反应的倾向增加,并且与非过敏女性相比,未能下调这些反应。这可能是导致过敏母亲所生婴儿过敏风险增加的一个因素。

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