妊娠期高血压疾病妇女的长期心血管风险：来自多基因风险评分的见解

IF 3.1 2区医学 Q1 OBSTETRICS & GYNECOLOGY

Acta Obstetricia et Gynecologica Scandinavica Pub Date : 2025-07-31 DOI:10.1111/aogs.70021

Anna Kivioja, Jaakko Tyrmi, Elli Toivonen, Heini Huhtala, FinnGen, Tiina Jääskeläinen, Johannes Kettunen, Tanja Saarela, Hannele Laivuori

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引用次数: 0

摘要

先兆子痫（PE）与心血管疾病（CVD）风险升高之间的关联已被充分证明。最近的PE全基因组关联研究进一步强调了它们可能的共同遗传背景。我们研究了妊娠期高血压疾病（HDP）的历史，包括PE表型和正常妊娠，结合PE （PE- prs）、高收缩压（SBP-PRS）、冠状动脉疾病（CAD-PRS）或中风（stroke- prs）的多基因风险评分（prs），如何影响CVD的风险。材料和方法：该研究在FinnGen队列中进行，共有213942名芬兰女性，包括8858名PE女性，17916名HDP女性和196026名产妇对照。PE女性包括在HDP表型中。参与者根据他们的prs分为三组：低（80%）遗传风险。正常妊娠和中度PRSs的妇女作为对照。结果：PE和PE、高收缩压、CAD和卒中的高遗传风险的妇女与正常妊娠和中等遗传风险的妇女相比，患CVD的风险显著增加。PE-PRS的CVD风险比为1.87，SBP-PRS为2.31，CAD-PRS为1.94，卒中- prs为2.07，p值均为2 × 10-16。在患有任何HDP的女性中也观察到类似的模式。在妊娠血压正常的妇女中，高遗传风险仅导致心血管疾病风险适度增加。PE-PRS相应的hr为1.07 (p = 5 × 10-5)， SBP-PRS为1.32，CAD-PRS为1.19，stroke-PRS为1.16 （p值均为2 × 10-16）。在所有四个PRSs中，PE和任何HDP对CVD风险的影响大于单独的遗传风险。心血管疾病风险的升高一直持续到80岁。结论：在患有PE或任何HDP的女性中，PE、高收缩压、CAD和卒中的高遗传风险进一步增加了CVD的总体风险。在妊娠血压正常的妇女中，高遗传风险只会导致心血管疾病风险的适度增加。在评估长期心血管疾病风险时，包括产科病史在内的临床风险评估似乎优于使用PRSs进行的遗传风险评估。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

Long-term cardiovascular risk in women with hypertensive disorders of pregnancy: Insights from polygenic risk scores

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Long-term cardiovascular risk in women with hypertensive disorders of pregnancy: Insights from polygenic risk scores

Introduction

The association between preeclampsia (PE) and an elevated risk of cardiovascular disease (CVD) is well documented. Recent genome-wide association studies of PE have further highlighted their possible common genetic background. We investigated how the history of hypertensive disorders of pregnancy (HDP), including the PE phenotype, and normotensive pregnancy, combined with polygenic risk scores (PRSs) for PE (PE-PRS), high systolic blood pressure (SBP-PRS), coronary artery disease (CAD-PRS) or stroke (stroke-PRS), affects the risk for CVD.

Material and Methods

The study was conducted in the FinnGen cohort of 213 942 Finnish women, including 8858 women with PE, 17916 women with any HDP, and 196 026 parous controls. PE women were included in the HDP phenotype. Participants were classified based on their PRSs into three groups: low (<20%), moderate (20–80%) and high (>80%) genetic risk. Women with normotensive pregnancies and moderate PRSs served as controls.

Results

Women with PE and a high genetic risk for PE, high SBP, CAD, and stroke had a significantly increased risk of CVD compared to women with normotensive pregnancies and a moderate genetic risk. The hazard ratios (HRs) for CVD were 1.87 for PE-PRS, 2.31 for SBP-PRS, 1.94 for CAD-PRS, and 2.07 for stroke-PRS, all p-values 2 × 10⁻¹⁶. A similar pattern was observed in women with any HDP. Among women with normotensive pregnancies, a high genetic risk led to only a modest increase in CVD risk. The corresponding HRs were 1.07 for PE-PRS (p = 5 × 10⁻⁵), 1.32 for SBP-PRS, 1.19 for CAD-PRS, and 1.16 for stroke-PRS (all p values 2 × 10⁻¹⁶). Across all four PRSs, the impact of PE and any HDP on CVD risk was greater than that of genetic risk alone. The elevated CVD risk persisted up to the age of 80.

Conclusions

In women with PE or any HDP, a high genetic risk for PE, high SBP, CAD, and stroke further increases the overall risk of CVD. Among women with normotensive pregnancies, a high genetic risk confers only a modest increase in CVD risk. In evaluating long-term CVD risk, clinical risk assessment, including obstetric history, appears to outperform genetic risk evaluation using PRSs.

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来源期刊

Acta Obstetricia et Gynecologica Scandinavica 医学-妇产科学

CiteScore

8.00

自引率

4.70%

发文量

180

审稿时长

3-6 weeks

期刊介绍： Published monthly, Acta Obstetricia et Gynecologica Scandinavica is an international journal dedicated to providing the very latest information on the results of both clinical, basic and translational research work related to all aspects of women’s health from around the globe. The journal regularly publishes commentaries, reviews, and original articles on a wide variety of topics including: gynecology, pregnancy, birth, female urology, gynecologic oncology, fertility and reproductive biology.