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Prenatal immunologic predictors of postpartum depressive symptoms: a prospective study for potential diagnostic markers.

机译:产后抑郁症状的产前免疫学预测因子:潜在诊断标志物的前瞻性研究。

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摘要

In postpartum depression (PPD), immunologic changes have been proposed to be involved in the disease pathology. The study evaluates the regulation of the innate and adaptive immune response over the course of late pregnancy and postpartum period and their association with the development of postpartum depressive symptoms. Furthermore, prenatal immunologic markers for a PPD were investigated. Hundred pregnant women were included. At 34th and 38th week of pregnancy as well as 2 days, 7 weeks and 6 months postpartum, immune parameters (neopterin, regulatory T cells, CXCR1, CCR2, MNP1 and CD11a) were measured by flow cytometry/ELISA, and the psychopathology was evaluated. We found that regulatory T cells were significantly increased prenatal (p=0.011) and postnatal (p=0.01) in mothers with postnatal depressive symptoms. The decrease in CXCR 1 after delivery was significantly higher in mother with postnatal depressive symptoms (p=0.032). Mothers with postnatal depressive symptoms showed already prenatal significantly elevated neopterin levels (p=0.049). Finally, regulatory T cells in pregnancy strongly predict postnatal depressive symptoms (p=0.004). The present study revealed that prenatal and postnatal immunologic parameters are associated with postpartum depressive symptoms in mothers. In addition, we found immune markers that could eventually be the base for a biomarker set that predicts postnatal depressive symptoms already during pregnancy.
机译:在产后抑郁症 (PPD) 中,免疫学变化被认为与疾病病理学有关。该研究评估了妊娠晚期和产后过程中先天性和适应性免疫反应的调节及其与产后抑郁症状发展的关联。此外,还研究了 PPD 的产前免疫标志物。包括100名孕妇。在妊娠第34周和第38周以及产后2天、7周和6个月,通过流式细胞术/ELISA测量免疫参数(新蝶呤、调节性T细胞、CXCR1、CCR2、MNP1和CD11a),并评估精神病理学。我们发现,在有产后抑郁症状的母亲中,产前(p=0.011)和产后(p=0.01)的调节性T细胞显著增加。在有产后抑郁症状的母亲中,分娩后CXCR 1的下降幅度显著更高(p=0.032)。有产后抑郁症状的母亲在产前已经表现出显著升高的新蝶呤水平(p=0.049)。最后,妊娠期调节性T细胞强烈预测产后抑郁症状(p=0.004)。本研究表明,产前和产后免疫参数与母亲的产后抑郁症状有关。此外,我们发现免疫标志物最终可能成为预测怀孕期间产后抑郁症状的生物标志物集的基础。

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