Diagnostic biomolecules and combination therapy for pre-eclampsia.

Jingqi Qi, Bingbing Wu, Xiuying Chen, Wei Wei, Xudong Yao
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引用次数: 2

Abstract

Pre-eclampsia (PE), associated with placental malperfusion, is the primary reason for maternal and perinatal mortality and morbidity that can cause vascular endothelial injury and multi-organ injury. Despite considerable research efforts, no pharmaceutical has been shown to stop disease progression. If women precisely diagnosed with PE can achieve treatment at early gestation, the maternal and fetal outcomes can be maximally optimized by expectant management. Current diagnostic approaches applying maternal characteristics or biophysical markers, including blood test, urine analysis and biophysical profile, possess limitations in the precise diagnosis of PE. Biochemical factor research associated with PE development has generated ambitious diagnostic targets based on PE pathogenesis and dissecting molecular phenotypes. This review focuses on current developments in biochemical prediction of PE and the corresponding interventions to ameliorate disease progression, aiming to provide references for clinical diagnoses and treatments.

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先兆子痫的诊断性生物分子及联合治疗。
先兆子痫(PE)与胎盘灌注不良相关,是孕产妇和围产期死亡和发病的主要原因,可引起血管内皮损伤和多器官损伤。尽管进行了大量的研究,但没有任何药物被证明可以阻止疾病的发展。如果准确诊断为PE的妇女能够在妊娠早期得到治疗,那么通过孕妇管理可以最大限度地优化母婴结局。目前的诊断方法采用母体特征或生物物理标记,包括血液检查、尿液分析和生物物理谱,在PE的精确诊断方面存在局限性。基于PE发病机制和解剖分子表型,与PE发展相关的生化因子研究产生了雄心勃勃的诊断目标。本文就PE的生化预测及相应干预措施改善病情进展的研究进展作一综述,旨在为临床诊断和治疗提供参考。
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