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Molecular Targets of Aspirin and Prevention of Preeclampsia and Their Potential Association with Circulating Extracellular Vesicles during Pregnancy

机译:阿司匹林和预防先兆子痫的分子靶标及其与妊娠期循环细胞外囊泡的联系

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摘要

Uncomplicated healthy pregnancy is the outcome of successful fertilization, implantation of embryos, trophoblast development and adequate placentation. Any deviation in these cascades of events may lead to complicated pregnancies such as preeclampsia (PE). The current incidence of PE is 2–8% in all pregnancies worldwide, leading to high maternal as well as perinatal mortality and morbidity rates. A number of randomized controlled clinical trials observed the association between low dose aspirin (LDA) treatment in early gestational age and significant reduction of early onset of PE in high-risk pregnant women. However, a substantial knowledge gap exists in identifying the particular mechanism of action of aspirin on placental function. It is already established that the placental-derived exosomes (PdE) are present in the maternal circulation from 6 weeks of gestation, and exosomes contain bioactive molecules such as proteins, lipids and RNA that are a “fingerprint” of their originating cells. Interestingly, levels of exosomes are higher in PE compared to normal pregnancies, and changes in the level of PdE during the first trimester may be used to classify women at risk for developing PE. The aim of this review is to discuss the mechanisms of action of LDA on placental and maternal physiological systems including the role of PdE in these phenomena. This review article will contribute to the in-depth understanding of LDA-induced PE prevention.
机译:健康妊娠的简单进行是成功受精,胚胎植入,滋养细胞发育和适当胎盘的结果。这些事件级联中的任何偏差都可能导致复杂的妊娠,例如先兆子痫(PE)。目前全世界所有怀孕中PE的发生率为2–8%,导致孕产妇以及围产期的死亡率和发病率很高。许多随机对照临床试验观察到,高风险孕妇在妊娠早期低剂量阿司匹林(LDA)治疗与PE的早期发作显着减少之间存在关联。但是,在确定阿司匹林对胎盘功能的特定作用机制时,存在很大的知识差距。已经确定,从妊娠6周开始,胎盘来源的外泌体(PdE)存在于母体循环中,并且外泌体含有生物活性分子,例如蛋白质,脂质和RNA,是其原始细胞的“指纹”。有趣的是,与正常怀孕相比,PE中的外来体水平更高,并且在妊娠前三个月期间PdE水平的变化可用于对有发展PE风险的妇女进行分类。这篇综述的目的是讨论LDA对胎盘和母体生理系统的作用机制,包括PdE在这些现象中的作用。这篇评论文章将有助于深入了解LDA诱导的PE预防。

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