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Blood laboratory testing for early prediction of preeclampsia: chasing the finish line or at the starting blocks?

机译:血液实验室检测预测预测:追逐终点线或在起始块处?

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Preeclampsia (PE) affects 2-8% of pregnancies worldwide, thus representing an important cause of maternal and neonatal morbidity, up to death. Many studies have been designed to identify putative biomarkers for accurate and timely diagnosing PE, but only some of them were focused on specific and sensitive biomarkers for early prediction of this life-threatening condition. In particular, some prospective studies aimed to investigate the predictive role of circulating biomarkers before 20 weeks of gestation in the general pregnant population yielded conflicting results. This article is hence centered on results obtained in studies investigating the predictive performances of angiogenic, anti-angiogenic, inflammatory, endocrine, and epigenetic biomarkers. The available evidence suggests that angiogenic and anti-angiogenic molecules, in particular the sFlt1:PIGF ratio, may be considered the biomarkers with the best diagnostic performance in the second trimester. However, doubts remain about their use in clinical settings before the 20th gestational week. Even lower evidence is available for other biomarkers, due to the fact that some positive results have not been confirmed in ensuing investigations, whereas unresolved analytical issues still contribute to make their clinical reliability rather questionable. Differential expression of microRNAs seems also a promising evidence for early prediction of PE, but additional research and well-designed prospective studies are needed to identify and validate routine predictive tests.
机译:Preclampsia(PE)影响全球2-8%的怀孕,从而代表母亲和新生儿发病率的重要原因,达到死亡。许多研究旨在识别推定的生物标志物,以便准确和及时诊断PE,但其中一些人专注于特定和敏感的生物标志物,以便早期预测这种危及生命的病情。特别是,一些前瞻性研究旨在调查循环生物标志物在妊娠一般孕腺群体20周之前循环生物标志物的预测作用产生的矛盾的结果。因此,本文以研究在研究研究血管生成,抗血管生成,炎症,内分泌和表观遗传生物标志物的预测性表演中获得的结果为中心。可用证据表明,血管生成和抗血管生成分子,特别是SFLT1:PIGF比,可以被认为是具有最佳诊断性能的生物标志物。然而,怀疑在第20期之前的临床环境中仍然在临床环境中使用。即使是较低的证据可用于其他生物标志物,因为某些积极的结果尚未在随后的调查中确认,而未解决的分析问题仍然有助于使其临床可靠性相当可疑。 MicroRNA的差异表达也是对PE的早期预测的有希望的证据,但需要额外的研究和设计精心设计的前瞻性研究来识别和验证常规预测性测试。

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