与生物标志物相关的胎儿生长限制研究进展

Liqun Sun
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引用次数: 1

摘要

摘要胎儿生长受限(FGR)在全球范围内的患病率约为10%,并与围产期死亡率和发病率的增加有关。FGR通常由胎盘功能不全引起,可早期开始(<32  周)或晚些时候(≥32  周)胎龄。假阳性的产前诊断可能导致不必要的监测和干预,并导致产妇焦虑。而假阴性诊断会使胎儿面临更高的死胎风险,并使妊娠不符合适当的护理和潜在的治疗条件。FGR妊娠的临床管理面临着决定最佳分娩时间的复杂挑战,因为目前的主要解决方案是尽早分娩,但医源性早产与不良的短期和长期结果有关。FGR的早期准确诊断有助于更好地分层临床管理,以及制定和实施治疗方案,最终有利于临床护理,并有可能改善短期和长期健康结果。这篇综述的目的是介绍胎盘功能不全的生物标志物的新见解,包括生物标志物在预测和预防FGR中的当前和潜在价值,并强调生物标志物与子宫内不良结果之间的联系,以探索胎儿生长受损的具体机制,为日后疾病奠定基础。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
The Update of Fetal Growth Restriction Associated with Biomarkers
Abstract Fetal growth restriction (FGR) has a prevalence of about 10% worldwide and is associated with an increased risk of perinatal mortality and morbidity. FGR is commonly caused by placental insufficiency and can begin early (<32  weeks) or in late (≥32  weeks) gestational age. A false positive antenatal diagnosis may lead to unnecessary monitoring and interventions, as well as cause maternal anxiety. Whereas a false negative diagnosis exposes the fetus to an increased risk of stillbirth and renders the pregnancy ineligible from the appropriate care and potential treatments. The clinical management of FGR pregnancies faces a complex challenge of deciding on the optimal timing of delivery as currently the main solution is to deliver the baby early, but iatrogenic preterm delivery of infants is associated with adverse short- and long-term outcomes. Early and accurate diagnosis of FGR could aid in better stratification of clinical management, and the development and implementation of treatment options, ultimately benefiting clinical care and potentially improving both short- and long-term health outcomes. The aim of this review is to present the new insights on biomarkers of placenta insufficiency, including their current and potential value of biomarkers in the prediction and prevention for FGR, and highlight the association between biomarkers and adverse outcomes in utero to explore the specific mechanism of impaired fetal growth that establish the basis for disease later in life.
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