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Differentially expressed microRNAs in maternal plasma for the noninvasive prenatal diagnosis of Down syndrome (trisomy 21).

机译:母体血浆中差异表达的微小RNA,可用于唐氏综合症的非侵入性产前诊断(21三体性)。

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摘要

OBJECTIVES: Most developmental processes are under the control of small regulatory RNAs called microRNAs (miRNAs). We hypothesize that different fetal developmental processes might be reflected by extracellular miRNAs in maternal plasma and may be utilized as biomarkers for the noninvasive prenatal diagnosis of chromosomal aneuploidies. In this proof-of-concept study, we report on the identification of extracellular miRNAs in maternal plasma of Down syndrome (DS) pregnancies. METHODS: Using high-throughput quantitative PCR (HT-qPCR), 1043 miRNAs were investigated in maternal plasma via comparison of seven DS pregnancies with age and fetal sex matched controls. RESULTS: Six hundred and ninety-five miRNAs were identified. Thirty-six significantly differentially expressed mature miRNAs were identified as potential biomarkers. Hierarchical cluster analysis of these miRNAs resulted in the clear discrimination of DS from euploid pregnancies. Gene targets of the differentially expressed miRNAs were enriched in signaling pathways such as mucin type-O-glycans, ECM-receptor interactions, TGF-beta, and endocytosis, which have been previously associated with DS. CONCLUSIONS: miRNAs are promising and stable biomarkers for a broad range of diseases and may allow a reliable, cost-efficient diagnostic tool for the noninvasive prenatal diagnosis of DS.
机译:目的:大多数发育过程都在称为微RNA(miRNA)的小型调节性RNA的控制下。我们假设母体血浆中的细胞外miRNA可能反映了不同的胎儿发育过程,并且可以用作染色体非整倍性的非侵入性产前诊断的生物标记。在此概念验证研究中,我们报告了唐氏综合症(DS)孕妇血浆中细胞外miRNA的鉴定。方法:采用高通量定量PCR(HT-qPCR),通过比较7名DS孕妇与年龄和胎儿性别匹配的对照,在孕妇血浆中研究了1043个miRNA。结果:鉴定出965个miRNA。三十六显着差异表达的成熟miRNA被确定为潜在的生物标志物。这些miRNA的层次聚类分析导致DS与整倍体妊娠的明显区别。差异表达的miRNA的基因靶点富含信号传导途径,如粘蛋白O型聚糖,ECM受体相互作用,TGF-β和胞吞作用,这些以前已与DS相关。结论:miRNA是广泛疾病的有前途和稳定的生物标志物,可能为DS的无创产前诊断提供可靠,经济高效的诊断工具。

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