Profiling Cytokines According to the Presence or Absence of Small-for-Gestational Age Using Amniotic Fluid Retrieved During Cesarean Section From Pregnant Women With Early-Onset Preeclampsia.

IF 2.3 3区医学 Q1 MEDICINE, GENERAL & INTERNAL

Journal of Korean Medical Science Pub Date : 2025-09-01 DOI:10.3346/jkms.2025.40.e213

Soyoung Shin, Shin Kim, Gisu Lee, Jingon Bae, Junho Kang, Jaehyun Park

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Abstract

Background: Preeclampsia (PE) is a hypertensive disorder and a major cause of maternal and fetal mortality. We aimed to investigate the molecular properties of early-onset PE, which requires delivery before 34 weeks' gestation by analyzing the molecular cytokine profile of amniotic fluid obtained during cesarean section from pregnant women with early-onset PE, based on the presence or absence of small-for-gestational age (SGA).

Methods: This study included 73 pregnant women with early-onset PE among which 21 women had SGA infants, whose birth weight was less than the 10th percentile of the gestational age-specific birth weight. Amniocentesis was performed after exposing the amniotic sac during cesarean delivery. Twenty-five cases of appropriate-for-gestational age (AGA) infants, who had birth weights between the 25th and 75th percentile of the gestational age-specific birth weight, were arbitrarily selected as a control group. Potential protein biomarkers were analyzed using the Olink® Explore 384 Inflammation panel with a Proximity Extension Assay technique. The biological implications of the differentially expressed proteins (DEPs) were assessed using the web-based tool Database for Annotation, Visualization, and Integrated Discovery 2021. Enrichment analysis of hub genes was performed using the Metascape Database.

Results: Although the mean birth weight was significantly lower in the SGA group than that in the AGA group (945.2 ± 302.3 vs. 1,590.0 ± 393.2, respectively; P < 0.001), no difference was observed in the mean gestational age at delivery (P > 0.05). Sixteen DEPs (EPO, WFIKKN2, CLSTN2, CSF3, COL9A1, SCG3, CCL23, SKAP2, CCL20, GZMB, TIMP3, FIS1, IL17C, PON3, VEGFA, and CXCL8) were found to be upregulated in the SGA group compared with the AGA group. Six hub genes (CCL20, CSF3, EPO, VEGFA, IL17C, and GZMB), which are mainly involved in cytokine-cytokine receptor interactions, were overexpressed in the SGA group.

Conclusion: We found six upregulated hub genes with potential as novel biomarkers for early-onset PE with SGA. Although further investigation is warranted to validate our results, our findings may contribute to a better understanding of the pathogenesis of early-onset PE with SGA.

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利用早发性子痫前期孕妇剖宫产术中提取的羊水分析存在或不存在小胎龄的细胞因子

背景：先兆子痫（PE）是一种高血压疾病，是孕产妇和胎儿死亡的主要原因。我们的目的是研究早发性PE的分子特性，早发性PE需要在妊娠34周之前分娩，通过分析剖宫产术中获得的早发性PE孕妇的羊水分子细胞因子谱，基于是否存在小胎龄（SGA）。方法：本研究纳入73例早发性PE孕妇，其中21例为SGA儿，其出生体重小于胎龄出生体重的第10百分位。剖宫产时暴露羊膜囊后进行羊膜穿刺术。随机选择25例胎龄适宜婴儿（AGA）作为对照组，这些婴儿的出生体重在胎龄特定出生体重的第25 - 75百分位之间。使用Olink®Explore 384炎症面板和邻近扩展测定技术分析潜在的蛋白质生物标志物。差异表达蛋白（DEPs）的生物学意义使用基于web的工具Database for Annotation， Visualization， and Integrated Discovery 2021进行评估。利用metscape数据库对枢纽基因进行富集分析。结果：SGA组的平均出生体重明显低于AGA组（945.2±302.3∶1590.0±393.2;P < 0.001），但分娩时平均胎龄差异无统计学意义（P < 0.05）。16个DEPs （EPO、WFIKKN2、CLSTN2、CSF3、COL9A1、SCG3、CCL23、SKAP2、CCL20、GZMB、TIMP3、FIS1、IL17C、PON3、VEGFA和CXCL8）在SGA组中与AGA组相比上调。6个主要参与细胞因子-细胞因子受体相互作用的枢纽基因（CCL20、CSF3、EPO、VEGFA、IL17C、GZMB）在SGA组中过表达。结论：我们发现了6个上调的中枢基因，它们可能成为早发性PE伴SGA的新生物标志物。虽然需要进一步的研究来验证我们的结果，但我们的发现可能有助于更好地理解早发性PE伴SGA的发病机制。

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来源期刊

Journal of Korean Medical Science 医学-医学：内科

CiteScore

7.80

自引率

8.90%

发文量

320

审稿时长

3-6 weeks

期刊介绍： The Journal of Korean Medical Science (JKMS) is an international, peer-reviewed Open Access journal of medicine published weekly in English. The Journal’s publisher is the Korean Academy of Medical Sciences (KAMS), Korean Medical Association (KMA). JKMS aims to publish evidence-based, scientific research articles from various disciplines of the medical sciences. The Journal welcomes articles of general interest to medical researchers especially when they contain original information. Articles on the clinical evaluation of drugs and other therapies, epidemiologic studies of the general population, studies on pathogenic organisms and toxic materials, and the toxicities and adverse effects of therapeutics are welcome.