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游离胎儿 DNA 作为预测子痫前期的有用标志物。

Cell-Free Foetal DNA as a Useful Marker for Preeclampsia Prediction.

机构信息

Maternity Department, National Medical Research Center for Obstetrics, Gynecology and Perinatology named after Academician V.I. Kulakov of Ministry of Healthcare of Russian Federation, Ac. Oparina str. 4, Moscow, Russia, 117997.

Federal State Autonomous Educational Institution of Higher Education, IM Sechenov First Moscow State Medical University of the Ministry of Health of the Russian Federation, Moscow, Russia.

出版信息

Reprod Sci. 2021 May;28(5):1563-1569. doi: 10.1007/s43032-021-00466-w. Epub 2021 Jan 21.

Abstract

Preeclampsia (PE) is a leading cause of maternal complications and is diagnosed by clinical manifestation. The aim of the study was to evaluate changes of cell-free DNA (cfDNA) and cell-free foetal DNA (cffDNA) concentration during uncomplicated pregnancy and PE in one group of women, and define the predictive value for PE. A total of 580 women were prospectively evaluated, 20 of them developed PE and were included in laboratory analysis, and 22 healthy pregnant with uncomplicated pregnancy were included as the laboratory control group. We determined cfDNA and cffDNA in maternal blood at 11-14, 24-26, and 30-32 weeks. Level of cfDNA was evaluated by determining the RASSF1A gene using PCR analysis, cffDNA-by determining the hypermethylated part of RASSF1A gene. The concentration of cfDNA did not differ in the first and second trimesters but significantly increased at 30-32 weeks in both groups. During uncomplicated pregnancy, median cffDNA level increased from 14.15 GE/ml to 24.87 GE/ml (p = 0.002) and 32.62 GE/ml (p = 0.005). In the PE group, an elevation in cffDNA level was significant only in the second half of pregnancy (from 54.85 to 96.72 (p > 0.05) and 158.30 GE/ml (p = 0.031) at 11-14, 24-26, and 30-32 weeks, respectively). At all studied periods, cffDNA level in the PE group was significantly higher compared to uncomplicated pregnancy (р < 0.001). ROC analysis showed that a cut-off value of cffDNA concentration 22.54 GE/ml in maternal blood at 11-14 weeks of pregnancy had the greatest predictive value for PE prediction, with 85.0% sensitivity and 81.8% specificity. CffDNA is a promising marker for PE prediction from the first trimester of pregnancy.

摘要

子痫前期 (PE) 是导致产妇并发症的主要原因,其诊断依据临床表现。本研究的目的是评估同一组女性在无并发症妊娠和 PE 期间游离 DNA (cfDNA) 和游离胎儿 DNA (cffDNA) 浓度的变化,并确定其对 PE 的预测价值。共前瞻性评估了 580 名女性,其中 20 名发生 PE 并纳入实验室分析,22 名健康孕妇纳入无并发症妊娠作为实验室对照组。我们在 11-14、24-26 和 30-32 周时检测了母体血液中的 cfDNA 和 cffDNA。通过 PCR 分析确定 RASSF1A 基因来评估 cfDNA 水平,通过确定 RASSF1A 基因的超甲基化部分来评估 cffDNA 水平。两组在第一和第二孕期的 cfDNA 浓度没有差异,但在两个孕期均在 30-32 周时显著增加。在无并发症妊娠中,cffDNA 水平从中值 14.15 GE/ml 增加到 24.87 GE/ml(p=0.002)和 32.62 GE/ml(p=0.005)。在 PE 组中,cffDNA 水平升高仅在妊娠后半期显著(从 54.85 增加到 96.72(p>0.05)和 158.30 GE/ml(p=0.031)在 11-14、24-26 和 30-32 周时)。在所有研究期间,PE 组的 cffDNA 水平明显高于无并发症妊娠(p<0.001)。ROC 分析显示,妊娠 11-14 周时母体血液中 cffDNA 浓度 22.54 GE/ml 的截断值对 PE 预测具有最大的预测价值,其敏感性为 85.0%,特异性为 81.8%。cffDNA 是预测妊娠早期 PE 的有前途的标志物。

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