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首页> 美国卫生研究院文献>Medicina >Mature miR-99a Upregulation in the Amniotic Fluid Samples from Female Fetus Down Syndrome Pregnancies: A Pilot Study
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Mature miR-99a Upregulation in the Amniotic Fluid Samples from Female Fetus Down Syndrome Pregnancies: A Pilot Study

机译:女性胎儿唐氏综合症孕妇羊水样本中成熟miR-99a上调:一项初步研究。

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Although Down syndrome is the most frequent aneuploidy, its pathogenic molecular mechanisms are not yet fully understood. The aim of our study is to quantify—by qRT-PCR—the expression levels of both the mature forms and the pri-miRNAs of the microRNAs resident on chromosome 21 (miR(21)) in the amniotic fluid samples from Down syndrome singleton pregnancies and to estimate the impact of the differentially expressed microRNAs on Down syndrome fetal heart and amniocytes transcriptomes. We collected amniotic fluid samples harvested by trained obstetricians as part of the second trimester screening/diagnostic procedure for aneuploidies to assess the trisomy 21 status by QF-PCR and karyotyping. Next, we evaluated—by Taqman qRT-PCR—the expression levels of both the mature forms and the pri-miRNA precursors of the microRNAs resident on chromosome 21 in amniotic fluid samples from singleton Down syndrome and euploid pregnancies. Further, we combined miRWalk 3.0 microRNA target prediction with GEO DataSets analysis to estimate the impact of hsa-miR-99a abnormal expression on Down syndrome heart and amniocytes transcriptome. We found a statistically significant up-regulation of the mature form of miR-99a, but not pri-miR-99a, in the amniotic fluid samples from Down syndrome pregnancies with female fetuses. GATHER functional enrichment analysis of miRWalk3.0-predicted targets from Down syndrome amniocytes and fetal hearts transcriptome GEODataSets outlined both focal adhesion and cytokine–cytokine receptor interaction signaling as novel signaling pathways impacted by miR-99a and associated with cardiac defects in female Down syndrome patients. The significant overexpression of miR-99a, but not pri-miR-99a, points towards an alteration of the post-transcriptional mechanisms of hsa-miR-99a maturation and/or stability in the female trisomic milieu, with a potential impact on signaling pathways important for proper development of the heart.
机译:尽管唐氏综合症是最常见的非整倍性,但其致病分子机制尚未完全了解。我们研究的目的是通过qRT-PCR定量分析唐氏综合征单胎孕妇羊水样本中驻留在21号染色体(miR(21))上的microRNA的成熟形式和pri-miRNA的表达水平。并评估差异表达的microRNA对唐氏综合症胎儿心脏和羊膜细胞转录组的影响。我们收集了受过训练的产科医生收集的羊水样本,作为非整倍性的中期妊娠筛查/诊断程序的一部分,以通过QF-PCR和核型分析评估21三体状态。接下来,我们通过Taqman qRT-PCR评估了来自单例唐氏综合征和整倍体妊娠的羊水样本中驻留在21号染色体上的microRNA的成熟形式和pri-miRNA前体的表达水平。此外,我们将miRWalk 3.0 microRNA靶标预测与GEO数据集分析相结合,以估计hsa-miR-99a异常表达对唐氏综合症心脏和羊膜细胞转录组的影响。我们发现女性唐氏综合症孕妇的羊水样本中,miR-99a的成熟形式(但不包含pri-miR-99a)的统计学显着上调。对唐氏综合症羊水和胎儿心脏转录组GEODataSets预测的miRWalk3.0靶标的GATHER功能富集分析概述了粘着斑和细胞因子-细胞因子受体相互作用的信号传导是miR-99a影响并与女性唐氏综合症患者心脏缺陷相关的新型信号传导途径。 miR-99a(而不是pri-miR-99a)的显着过表达表明hsa-miR-99a转录后机制在女性三体环境中成熟和/或稳定性的改变,可能会对信号传导途径产生影响对于心脏的正常发育很重要。

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