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追踪子痫前期的脂质指纹图谱。

Tracing the Lipid Fingerprints of Preeclampsia.

作者信息

Vaishya Suniti, Joshi Sadhana Ramchandra

机构信息

Mother and Child Health, ICMR-Collaborating Centre for Excellence (ICMR-CCoE), Interactive Research School for Health Affairs, Bharati Vidyapeeth (Deemed to be University), Pune Satara Road, Pune, 411043, India.

出版信息

Reprod Sci. 2025 Jan;32(1):52-63. doi: 10.1007/s43032-024-01731-4. Epub 2024 Oct 30.

Abstract

Preeclampsia (PE) is the most common pregnancy-related complication responsible for maternal mortality and morbidity. PE pathogenesis is characterized by placental dysfunction, impaired invasion of trophoblast, and defective spiral artery remodelling. Even after many years of research on PE, the etiology and pathophysiology of PE is still elusive. Our earlier studies have shown deregulated maternal and placental fatty acid and lipid metabolism to be associated with the pathogenesis of PE. Currently available lipidomics data have shown that glycerophospholipids, sphingolipid and cholesterol metabolism are mainly altered in preeclampsia. Including these five metabolites (SM C28:1, SM C30:1, LPC C19:0, LPE C20:0, propane-1,3-diol) with currently used protein biomarkers like sFlt-1/PlGF will improve PE prediction. Similarly, CE17:1 and CER(d20:1/24:1) alongwith sFlt-1/PlGF makes a better prediction of PE than sFlt-1/PlGF alone A comprehensive map of lipid profiles in early pregnancy may provide an improved understanding of disease pathogenesis and will be useful predictive biomarkers. In this article, we aimed to summarize the significance of lipid metabolism in the preeclampsia pathogenesis and altered lipidome signatures in preeclampsia. We also discuss the future scope of lipidomics in aiding early prediction of PE and future cardiovascular risk in both mother and child.

摘要

子痫前期(PE)是导致孕产妇死亡和发病的最常见妊娠相关并发症。PE的发病机制以胎盘功能障碍、滋养细胞浸润受损和螺旋动脉重塑缺陷为特征。尽管对PE进行了多年研究,但其病因和病理生理学仍不清楚。我们早期的研究表明,母体和胎盘脂肪酸及脂质代谢失调与PE的发病机制有关。目前可用的脂质组学数据显示,甘油磷脂、鞘脂和胆固醇代谢在子痫前期主要发生改变。将这五种代谢物(SM C28:1、SM C30:1、LPC C19:0、LPE C20:0、丙烷 - 1,3 - 二醇)与目前使用的蛋白质生物标志物如sFlt - 1/PlGF相结合,将改善对子痫前期的预测。同样,CE17:1和CER(d20:1/24:1)与sFlt - 1/PlGF一起比单独使用sFlt - 1/PlGF能更好地预测子痫前期。早孕期脂质谱的综合图谱可能有助于更好地理解疾病发病机制,并将成为有用的预测生物标志物。在本文中,我们旨在总结脂质代谢在子痫前期发病机制中的意义以及子痫前期脂质组特征的改变。我们还讨论了脂质组学在辅助子痫前期早期预测以及母婴未来心血管风险方面的未来前景。

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