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基于炎症相关血浆蛋白的组合,对 34 孕周前自发性早产进行早期预测。

Early prediction of spontaneous preterm birth before 34 gestational weeks based on a combination of inflammation-associated plasma proteins.

机构信息

Department of Obstetrics and Gynecology, Region Kalmar County, Kalmar, Sweden.

Department of Biomedical and Clinical Sciences, Linköping University, Linköping, Sweden.

出版信息

Front Immunol. 2024 Jul 15;15:1415016. doi: 10.3389/fimmu.2024.1415016. eCollection 2024.

Abstract

BACKGROUND

In order to identify and possibly offer prophylactic treatment to women at risk for preterm birth (PTB), novel prediction models for PTB are needed. Our objective was to utilize high-sensitive plasma protein profiling to investigate whether early prediction of spontaneous PTB (sPTB) before 34 gestational weeks (gw) was possible in a low-risk population.

METHODS

A case-control study was conducted on 46 women with sPTB before 34 gw and 46 women with normal pregnancies and term deliveries. Prospectively collected plasma sampled at gw 11 (range 7-16) and gw 25 (range 23-30) was analyzed with a high-sensitivity Proximity Extension Assay for levels of 177 inflammation-associated proteins, and statistically processed with multivariate logistic regression analysis.

RESULTS

In the first trimester, higher levels of hepatocyte growth factor (HGF) were associated with sPTB <34 gw (OR 1.49 (1.03-2.15)). In the second trimester, higher levels of interleukin (IL)-10 (OR 2.15 (1.18-3.92)), IL-6 (OR 2.59 (1.34-4.99)), and the receptor activator of nuclear factor κB (RANK) (OR 2.18 (1.26-3.77)) were associated with sPTB <34 gw. The area under the curve for the prediction models including these proteins was 0.653 (0.534-0.759) in the first trimester and 0.854 (0.754-0.925) in the second trimester.

CONCLUSION

A combination of inflammation-associated plasma proteins from the second trimester of pregnancy showed a good predictive ability regarding sPTB before 34 gw, suggesting it could be a valuable supplement for the assessment of the clinical risk of sPTB. However, although a high number (n=177) of plasma proteins were analyzed with a high-sensitivity method, the prediction of sPTB in the first trimester remains elusive.

摘要

背景

为了识别和可能为早产(PTB)高危女性提供预防性治疗,需要新的 PTB 预测模型。我们的目的是利用高敏感的血浆蛋白谱来研究在低危人群中是否可以在 34 孕周(gw)之前早期预测自发性早产(sPTB)。

方法

对 46 例 34 gw 前 sPTB 孕妇和 46 例正常妊娠和足月分娩孕妇进行病例对照研究。前瞻性收集 11 gw(范围 7-16)和 25 gw(范围 23-30)采集的血浆样本,用高灵敏度的临近延伸分析检测 177 种炎症相关蛋白的水平,并进行多变量逻辑回归分析。

结果

在孕早期,较高的肝细胞生长因子(HGF)水平与 sPTB<34 gw 相关(OR 1.49(1.03-2.15))。在孕中期,较高的白细胞介素(IL)-10(OR 2.15(1.18-3.92))、IL-6(OR 2.59(1.34-4.99))和核因子κB 受体激活剂(RANK)(OR 2.18(1.26-3.77))水平与 sPTB<34 gw 相关。包含这些蛋白的预测模型的曲线下面积在孕早期为 0.653(0.534-0.759),在孕中期为 0.854(0.754-0.925)。

结论

来自妊娠中期的炎症相关血浆蛋白的组合对 34 gw 前 sPTB 具有良好的预测能力,表明其可能是评估 sPTB 临床风险的有价值的补充。然而,尽管使用高灵敏度方法分析了大量(n=177)血浆蛋白,但在孕早期仍无法预测 sPTB。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5e52/11284114/07e860fc32e5/fimmu-15-1415016-g001.jpg

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