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胎盘外泌体:理解妊娠并发症的替代指标。

Placental exosomes: A proxy to understand pregnancy complications.

机构信息

Department of Obstetrics and Gynecology, Division of Maternal-Fetal Medicine and Perinatal Research, The University of Texas Medical Branch at Galveston, Galveston, TX, USA.

Department of Gynaecology and Obstetrics, NanFang Hospital, Southern Medical University, Guangzhou, China.

出版信息

Am J Reprod Immunol. 2018 May;79(5):e12788. doi: 10.1111/aji.12788. Epub 2017 Nov 28.

Abstract

Exosomes (30- to 150-nm particles), originating from multivesicular bodies by the invagination of the endosomal membrane, are communication channels between cells. Exosomes are released by various cell types and cargo proteins, lipids, and nucleic acids reflecting the physiologic status of their cells of origin and cause functional changes in recipient cells, which are likely dependent on their quantity and/or cargo contents. Recently, placental exosomes, produced by various placental cell types, have been isolated from maternal blood using the placental protein-specific marker, placental alkaline phosphatase (PLAP). PLAP-positive exosomes are seen in maternal blood as early as the first trimester of pregnancy and increase as gestation progresses, with maximum numbers seen at term. Although the functional relevance of placental exosomes is still under investigation, several studies have linked placental exosomes changes (quantity and cargo) reflecting placental dysfunctions associated with adverse pregnancy events. As placental exosomes can be isolated from maternal blood, they are liquid biopsies reflecting placental functions. Hence, they are useful as biomarkers of placental functions and dysfunctions obtainable through non-invasive approaches. This review summarizes the biogenesis, release, and functions of exosomes and specifically expounds the role of placental-specific exosomes and their significance associated with pregnancy complications.

摘要

外泌体(30-150nm 大小的颗粒)起源于多泡体,通过内陷内体膜而形成,是细胞间的通讯通道。外泌体由各种细胞类型释放,其携带的货物(蛋白质、脂质和核酸)反映了它们来源细胞的生理状态,并导致受体细胞发生功能变化,这种变化可能依赖于它们的数量和/或货物内容。最近,使用胎盘蛋白特异性标志物胎盘碱性磷酸酶(PLAP),已经从母体血液中分离出各种胎盘细胞类型产生的胎盘外泌体。PLAP 阳性的外泌体在妊娠早期的第一个三个月就可见于母体血液中,并随着妊娠的进展而增加,足月时数量最多。虽然胎盘外泌体的功能相关性仍在研究中,但已有几项研究将胎盘外泌体的变化(数量和货物)与与不良妊娠事件相关的胎盘功能障碍联系起来。由于胎盘外泌体可以从母体血液中分离出来,因此它们是液体活检,可以反映胎盘功能。因此,它们可用作通过非侵入性方法获得的胎盘功能和功能障碍的生物标志物。本文综述了外泌体的生物发生、释放和功能,并特别阐述了胎盘特异性外泌体及其与妊娠并发症相关的意义。

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