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膜保护的凋亡滋养层微粒含有核酸:与子痫前期的相关性。

Membrane protected apoptotic trophoblast microparticles contain nucleic acids: relevance to preeclampsia.

作者信息

Orozco Aaron F, Jorgez Carolina J, Horne Cassandra, Marquez-Do Deborah A, Chapman Matthew R, Rodgers John R, Bischoff Farideh Z, Lewis Dorothy E

机构信息

Department of Immunology, Baylor College of Medicine, Houston, TX, USA.

出版信息

Am J Pathol. 2008 Dec;173(6):1595-608. doi: 10.2353/ajpath.2008.080414. Epub 2008 Oct 30.

Abstract

Microparticles (MPs) that circulate in blood may be a source of DNA for molecular analyses, including prenatal genetic diagnoses. Because MPs are heterogeneous in nature, however, further characterization is important before use in clinical settings. One key question is whether DNA is either bound to aggregates of blood proteins and lipid micelles or intrinsically associated with MPs from dying cells. To test the latter hypothesis, we asked whether MPs derived in vitro from dying cells were similar to those in maternal plasma. JEG-3 cells model extravillous trophoblasts, which predominate during the first trimester of pregnancy when prenatal diagnosis is most relevant. MPs were derived from apoptosis and increased over 48 hours. Compared with necrotic MPs, DNA in apoptotic MPs was more fragmented and resistant to plasma DNases. Membrane-specific dyes indicated that apoptotic MPs had more membranous material, which protects nucleic acids, including RNA. Flow cytometry showed that MPs derived from dying cells displayed light scatter and DNA staining similar to MPs found in maternal plasma. Quantification of maternal MPs using characteristics defined by MPs generated in vitro revealed a significant increase of DNA(+) MPs in the plasma of women with preeclampsia compared with plasma from women with normal pregnancies. Apoptotic MPs are therefore a likely source of stable DNA that could be enriched for both early genetic diagnosis and monitoring of pathological pregnancies.

摘要

血液中循环的微粒(MPs)可能是用于分子分析(包括产前基因诊断)的DNA来源。然而,由于MPs本质上具有异质性,在临床应用前进行进一步表征很重要。一个关键问题是DNA是与血液蛋白质和脂质微团的聚集体结合,还是与来自死亡细胞的MPs内在相关。为了验证后一种假设,我们研究了体外从死亡细胞衍生的MPs是否与母血中的MPs相似。JEG-3细胞模拟绒毛外滋养层细胞,在产前诊断最相关的妊娠早期占主导地位。MPs由凋亡产生,并在48小时内增加。与坏死性MPs相比,凋亡性MPs中的DNA片段化程度更高,且对血浆脱氧核糖核酸酶具有抗性。膜特异性染料表明,凋亡性MPs具有更多的膜性物质,可保护包括RNA在内的核酸。流式细胞术显示,来自死亡细胞的MPs呈现出与母血中发现的MPs相似的光散射和DNA染色。利用体外产生的MPs所定义的特征对母血MPs进行定量分析,结果显示,与正常妊娠女性的血浆相比,子痫前期女性血浆中DNA(+) MPs显著增加。因此,凋亡性MPs可能是稳定DNA的来源,可用于早期基因诊断和病理性妊娠监测。

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