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复发性流产患者中促凝的内皮细胞和组织因子表达的微颗粒升高。

Elevated procoagulant endothelial and tissue factor expressing microparticles in women with recurrent pregnancy loss.

机构信息

Department of Haemostasis and Thrombosis, National Institute of Immunohaematology (ICMR), KEM Hospital, Parel, Mumbai, India.

出版信息

PLoS One. 2013 Nov 20;8(11):e81407. doi: 10.1371/journal.pone.0081407. eCollection 2013.

Abstract

BACKGROUND

15% of reproducing couples suffer from pregnancy loss(PL) and recurs in 2-3%. One of the most frequently hypothesized causes of unexplained PL refers to a defective maternal haemostatic response leading to uteroplacental thrombosis. Hereditary thrombophilia and antiphospholipid antibodies have been extensively described as risk factors for PL in women with unknown aetiology. Recently, a new marker has emerged: the cell-derived procoagulant circulating microparticles(MPs) which have been reported to have a major role in many thrombosis complicated diseases. This study aims to analyze the significance of procoagulant MPs in women suffering from unexplained recurrent pregnancy loss(RPL), and characterize their cellular origin.

METHOD AND FINDINGS

115 women with RPL were analyzed for common thrombophilia markers and different cell derived MPs-total annexinV, platelet(CD41a), endothelial(CD146,CD62e), leukocyte(CD45), erythrocyte(CD235a) and tissue factor(CD142)(TF) expressing MPs and were compared with 20 healthy non-pregnant women. Methodology for MP analysis was standardized by participating in the "Vascular Biology Scientific and Standardization Committee workshop".

RESULTS

Total annexinV, TF and endothelial MPs were found significantly increased(p<0.05, 95% confidence interval) in women with RPL. The procoagulant activity of MPs measured by STA-PPL clotting time assay was found in correspondence with annexinV MP levels, wherein the clot time was shortened in samples with increased MP levels. Differences in platelet, leukocyte and erythrocyte derived MPs were not significant. Thirty seven of 115 women were found to carry any of the acquired or hereditary thrombophilia markers. No significant differences were seen in the MP profile of women with and without thrombophilia marker.

CONCLUSION

The presence of elevated endothelial, TF and phosphatidylserine expressing MPs at a distance (at least 3 months) from the PL suggests a continued chronic endothelial damage/activation which may get exaggerated at the onset of pregnancy. The data suggests that MPs may contribute to uteroplacental thrombosis and are associated with the pathogenesis of RPL.

摘要

背景

15%的妊娠夫妇会经历妊娠丢失(PL),其中 2-3%会复发。导致不明原因 PL 的最常见假设原因之一是母体止血反应缺陷导致胎盘血栓形成。遗传性血栓形成倾向和抗磷脂抗体已被广泛描述为不明病因 PL 女性的危险因素。最近,出现了一种新的标志物:细胞来源的促凝血循环微粒(MPs),据报道,它们在许多血栓形成相关疾病中起主要作用。本研究旨在分析患有不明原因复发性妊娠丢失(RPL)的妇女中促凝血 MPs 的意义,并对其细胞来源进行特征描述。

方法和发现

对 115 名 RPL 妇女进行了常见血栓形成倾向标志物和不同细胞来源 MPs(总 annexinV、血小板(CD41a)、内皮(CD146、CD62e)、白细胞(CD45)、红细胞(CD235a)和组织因子(CD142)(TF)表达 MPs)分析,并与 20 名健康未怀孕妇女进行比较。通过参加“血管生物学科学和标准化委员会研讨会”对 MPs 分析方法进行了标准化。

结果

发现 RPL 妇女中总 annexinV、TF 和内皮 MPs 显著增加(p<0.05,95%置信区间)。通过 STA-PPL 凝血时间测定法测量 MPs 的促凝血活性与 annexinV MP 水平相对应,其中 MPs 水平升高的样本中凝血时间缩短。血小板、白细胞和红细胞来源 MPs 的差异不显著。在 115 名妇女中,有 37 名发现携带任何获得性或遗传性血栓形成倾向标志物。有或没有血栓形成倾向标志物的妇女的 MPs 谱没有显著差异。

结论

在距离 PL 至少 3 个月的时间点,升高的内皮、TF 和磷脂酰丝氨酸表达 MPs 的存在表明持续的慢性内皮损伤/激活,在妊娠开始时可能会加剧。数据表明 MPs 可能导致胎盘血栓形成,并与 RPL 的发病机制相关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a195/3835417/1a10ba4edf5e/pone.0081407.g001.jpg

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