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足月自发性分娩前外周白细胞迁移的激活。

Activation of peripheral leukocyte migration before spontaneous labor at term.

机构信息

Department of Physiology, University of Alberta, Edmonton, Canada.

Department of Obstetrics and Gynecology, Faculty of Medicine, Juntendo University, Tokyo, Japan.

出版信息

Am J Obstet Gynecol. 2024 Nov;231(5):539.e1-539.e13. doi: 10.1016/j.ajog.2024.02.280. Epub 2024 Jun 5.

Abstract

BACKGROUND

Leukocytes are induced to migrate into the uterus at parturition, releasing cytokines and chemokines that activate it for delivery. A specific chemotactic signal is required for these actions, and published evidence suggests that it comes from the human fetal membranes and has a time-dependent component (ie, cells obtained at term in labor migrate more than cells obtained at term not yet in labor). The hypothesis that the fetal membrane chemoattractants activate the leukocytes to become responsive for migration was tested.

OBJECTIVE

This study aimed to: (1) examine the changes in leukocyte migration-responsiveness longitudinally from the late third trimester, to in labor, to 3 days postpartum; (2) explore the specific week-to-week changes in migration before delivery; (3) define the timing of chemokine receptor expression patterns in leukocytes relative to migration and the changes in cytokine and chemokine concentrations in maternal serum; (4) examine the ability of term fetal membrane-conditioned medium and term maternal serum to increase cell responsiveness; and (5) test the potential of the leukocyte migration assay to predict delivery within 1 week.

STUDY DESIGN

Leukocyte migration in response to a chemoattractive extract of term human fetal membranes was studied using a modified Boyden chamber. Flow cytometry assessed migrated cell phenotypes. The relationship between the expression of chemokine receptors and migration was tested using quantitative polymerase chain reaction, the bioassay, and regression analyses. Cytokines and chemokines in maternal serum were quantified using multiplex analysis. Conditioned medium from fetal membrane explants and maternal serum were evaluated for their abilities to enhance leukocyte migration using the bioassay. The ability of the bioassay to predict term delivery was assessed using receiver-operating characteristic curve and cost-curve analysis.

RESULTS

The number of leukocytes that migrated at term delivery was increased relative to the late third trimester, followed by a significant fall in numbers that migrated at 3 days postpartum (P=.002). The largest increase in migrated cells occurred 1 to 2 weeks before delivery. The messenger RNA abundance of several chemokine receptors increased in peripheral leukocytes at term in labor relative to the third trimester, and this correlated with an increase in migrated cells in 5 of 6 cases (R=0.589 to 0.897; P<.03). The concentrations of several chemokines and cytokines in maternal serum increased with labor onset. Fetal membrane explant-conditioned medium and maternal serum obtained at term labor increased the responsiveness of leukocytes to fetal membrane chemoattractive extract. The bioassay was demonstrated to predict delivery within 7 days with excellent performance characteristics using a cohort prevalence of 71.7% (positive predictive value=96.1%; negative predictive value=58.5%; sensitivity=74.2%; specificity=92.3%; positive likelihood ratio=9.25; and negative likelihood ratio=0.28). A single determination was validated to have a high degree of confidence.

CONCLUSION

Term human fetal membranes release chemoattractants near the end of pregnancy that increase in ability to activate and attract an increasing number of leukocytes as gestation advances.

摘要

背景

白细胞在分娩时被诱导迁移到子宫内,释放细胞因子和趋化因子,使子宫为分娩做好准备。这些作用需要特定的趋化信号,已有研究表明这种信号来自于人类胎膜,并具有时间依赖性成分(即,分娩时从足月胎盘中获得的细胞比尚未分娩的足月胎盘中获得的细胞迁移更多)。本研究旨在检验胎膜趋化因子激活白细胞以使其对迁移产生反应的假说。

目的

本研究旨在:(1)从妊娠晚期、分娩时到产后 3 天,纵向检测白细胞迁移反应性的变化;(2)探讨分娩前每周迁移的具体变化;(3)确定白细胞趋化因子受体表达模式与迁移以及母体血清细胞因子和趋化因子浓度变化之间的关系;(4)检测足月胎膜条件培养基和足月母体血清增加细胞反应性的能力;(5)测试白细胞迁移测定法预测 1 周内分娩的可能性。

研究设计

使用改良 Boyden 室研究了足月人胎膜趋化性提取物对白细胞迁移的反应。流式细胞术评估了迁移细胞的表型。使用定量聚合酶链反应、生物测定和回归分析来检测趋化因子受体的表达与迁移之间的关系。使用多重分析检测母体血清中的细胞因子和趋化因子。使用生物测定评估胎膜外植体条件培养基和母体血清增强白细胞迁移的能力。使用受试者工作特征曲线和成本曲线分析评估生物测定预测足月分娩的能力。

结果

分娩时迁移的白细胞数量与妊娠晚期相比增加,随后在产后 3 天数量显著下降(P=.002)。最大的迁移细胞增加发生在分娩前 1 至 2 周。与妊娠晚期相比,处于劳动状态的足月时外周白细胞中几种趋化因子受体的信使 RNA 丰度增加,在 6 例中有 5 例(R=0.589 至 0.897;P<.03)与迁移细胞增加相关。母体血清中几种趋化因子和细胞因子的浓度随分娩开始而增加。胎膜外植体条件培养基和足月分娩时获得的母体血清增加了白细胞对胎膜趋化性提取物的反应能力。生物测定法在队列患病率为 71.7%的情况下,具有出色的性能特征,可在 7 天内预测分娩(阳性预测值=96.1%;阴性预测值=58.5%;灵敏度=74.2%;特异性=92.3%;阳性似然比=9.25;阴性似然比=0.28)。单次测定具有高度置信度。

结论

足月人胎膜在妊娠末期释放趋化因子,随着妊娠的进展,趋化因子激活和吸引越来越多白细胞的能力增加。

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