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首页> 外文期刊>Hypertension: An Official Journal of the American Heart Association >Early Pregnancy Prediction of Preeclampsia in Nulliparous Women, Combining Clinical Risk and BiomarkersNovelty and Significance
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Early Pregnancy Prediction of Preeclampsia in Nulliparous Women, Combining Clinical Risk and BiomarkersNovelty and Significance

机译:结合临床风险和生物标志物,对多核妇女先兆子痫的早期妊娠预测

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More than half of all cases of preeclampsia occur in healthy first-time pregnant women. Our aim was to develop a method to predict those at risk by combining clinical factors and measurements of biomarkers in women recruited to the Screening for Pregnancy Endpoints (SCOPE) study of low-risk nulliparous women. Forty-seven biomarkers identified on the basis of (1) association with preeclampsia, (2) a biological role in placentation, or (3) a role in cellular mechanisms involved in the pathogenesis of preeclampsia were measured in plasma sampled at 14 to 16 weeks’ gestation from 5623 women. The cohort was randomly divided into training (n=3747) and validation (n=1876) cohorts. Preeclampsia developed in 278 (4.9%) women, of whom 28 (0.5%) developed early-onset preeclampsia. The final model for the prediction of preeclampsia included placental growth factor, mean arterial pressure, and body mass index at 14 to 16 weeks’ gestation, the consumption of ≥3 pieces of fruit per day, and mean uterine artery resistance index. The area under the receiver operator curve (95% confidence interval) for this model in training and validation cohorts was 0.73 (0.70–0.77) and 0.68 (0.63–0.74), respectively. A predictive model of early-onset preeclampsia included angiogenin/placental growth factor as a ratio, mean arterial pressure, any pregnancy loss <10 weeks, and mean uterine artery resistance index (area under the receiver operator curve [95% confidence interval] in training and validation cohorts, 0.89 [0.78–1.0] and 0.78 [0.58–0.99], respectively). Neither model included pregnancy-associated plasma protein A, previously reported to predict preeclampsia in populations of mixed parity and risk. In nulliparous women, combining multiple biomarkers and clinical data provided modest prediction of preeclampsia.# Novelty and Significance {#article-title-41}
机译:在所有先兆子痫病例中,一半以上发生在健康的初次怀孕的孕妇中。我们的目标是开发一种方法,通过将临床因素与生物标志物的测定相结合来预测低危未产妇的妊娠终点筛查(SCOPE),从而预测这些人群的风险。在14至16周的血浆中测定了47种生物标志物,这些标志物是基于(1)与子痫前期的关联,(2)胎盘的生物学作用或(3)在子痫前期发病机理中涉及的细胞机制中的作用而确定的来自5623名妇女的妊娠。将该队列随机分为训练(n = 3747)和验证(n = 1876)队列。子痫前期发生在278名(4.9%)妇女中,其中28名(0.5%)发生了早发型先兆子痫。预测先兆子痫的最终模型包括胎盘生长因子,平均动脉压和妊娠14至16周时的体重指数,每天消耗≥3颗水果以及平均子宫动脉阻力指数。在训练和验证队列中,此模型的接收者操作符曲线下的面积(95%置信区间)分别为0.73(0.70-0.77)和0.68(0.63-0.74)。早发先兆子痫的预测模型包括血管生成素/胎盘生长因子,比率,平均动脉压,任何妊娠流产<10周以及平均子宫动脉阻力指数(接受者操作者曲线下的面积[95 %置信区间]在训练和验证队列中,分别为0.89 [0.78–1.0]和0.78 [0.58–0.99]。两种模型均未包含与妊娠相关的血浆蛋白A,先前曾报道过这种蛋白可预测先兆子痫在混合胎和风险人群中的发生。在未产妇中,结合多种生物标记物和临床数据可对先兆子痫做出适度的预测。#新颖性和意义{#article-title-41}

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