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用于在孕五周时检测胎儿基因组和评估妊娠健康状况的宫颈滋养层细胞。

Endocervical trophoblast for interrogating the fetal genome and assessing pregnancy health at five weeks.

作者信息

Kadam Leena, Jain Chandni, Kohan-Ghadr Hamid Reza, Krawetz Stephen A, Drewlo Sascha, Armant D Randall

机构信息

Department of Obstetrics and Gynecology, Wayne State University, Detroit, MI, United States.

Department of Obstetrics, Gynecology and Reproductive Biology, College of Human Medicine, Michigan State University, Grand Rapids, MI, USA.

出版信息

Eur J Med Genet. 2019 Aug;62(8):103690. doi: 10.1016/j.ejmg.2019.103690. Epub 2019 Jun 18.

Abstract

Prenatal testing for fetal genetic traits and risk of obstetrical complications is essential for maternal-fetal healthcare. The migration of extravillous trophoblast (EVT) cells from the placenta into the reproductive tract and accumulation in the cervix offers an exciting avenue for prenatal testing and monitoring placental function. These cells are obtained with a cervical cytobrush, a routine relatively safe clinical procedure during pregnancy, according to published studies and our own observations. Trophoblast retrieval and isolation from the cervix (TRIC) obtains hundreds of fetal cells with >90% purity as early as five weeks of gestation. TRIC can provide DNA for fetal genotyping by targeted next-generation sequencing with single-nucleotide resolution. Previously, we found that known protein biomarkers are dysregulated in EVT cells obtained by TRIC in the first trimester from women who miscarry or later develop intrauterine growth restriction or preeclampsia. We have now optimized methods to stabilize RNA during TRIC for subsequent isolation and analysis of trophoblast gene expression. Here, we report transcriptomics analysis demonstrating that the expression profile of TRIC-isolated trophoblast cells was distinct from that of maternal cervical cells and included genes associated with the EVT phenotype and invasion. Because EVT cells are responsible for remodeling the maternal arteries and their failure is associated with pregnancy disorders, their molecular profiles could reflect maternal risk, as well as mechanisms underlying these disorders. The use of TRIC to analyze EVT genomes, transcriptomes and proteomes during ongoing pregnancies could provide new tools for anticipating and managing both fetal genetic and maternal obstetric disorders.

摘要

对胎儿遗传特征和产科并发症风险进行产前检测对于母婴保健至关重要。绒毛外滋养层(EVT)细胞从胎盘迁移到生殖道并在宫颈中积聚,为产前检测和监测胎盘功能提供了一个令人兴奋的途径。根据已发表的研究和我们自己的观察,这些细胞是通过宫颈细胞刷获取的,这是孕期一种常规且相对安全的临床操作。从宫颈获取和分离滋养层细胞(TRIC)早在妊娠五周时就能获得数百个纯度>90%的胎儿细胞。TRIC可以通过具有单核苷酸分辨率的靶向新一代测序为胎儿基因分型提供DNA。此前,我们发现已知的蛋白质生物标志物在孕早期通过TRIC从流产或后来发生胎儿生长受限或先兆子痫的女性中获得的EVT细胞中表达失调。我们现在已经优化了TRIC过程中RNA的稳定方法,以便随后分离和分析滋养层基因表达。在此,我们报告转录组学分析表明,TRIC分离的滋养层细胞的表达谱与母体宫颈细胞不同,包括与EVT表型和侵袭相关的基因。由于EVT细胞负责重塑母体动脉,其功能障碍与妊娠疾病相关,它们的分子谱可能反映母体风险以及这些疾病的潜在机制。在持续妊娠期间使用TRIC分析EVT基因组、转录组和蛋白质组可以为预测和管理胎儿遗传疾病和母体产科疾病提供新工具。

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