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Systems biology evaluation of cell-free amniotic fluid transcriptome of term and preterm infants to detect fetal maturity

机译:足月和早产儿无细胞羊水转录组的系统生物学评估,以检测胎儿成熟度

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Background Amniotic fluid (AF) is a proximal fluid to the fetus containing higher amounts of cell-free fetal RNA/DNA than maternal serum, thereby making it a promising source for identifying novel biomarkers that predict fetal development and organ maturation. Our aim was to compare AF transcriptomic profiles at different time points in pregnancy to demonstrate unique genetic signatures that would serve as potential biomarkers indicative of fetal maturation. Methods We isolated AF RNA from 16 women at different time points in pregnancy: 4 from 18 to 24 weeks, 6 from 34 to 36 weeks, and 6 from 39 to 40 weeks. RNA-sequencing was performed on cell-free RNA. Gene expression and splicing analyses were performed in conjunction with cell-type and pathway predictions. Results Sample-level analysis at different time points in pregnancy demonstrated a strong correlation with cell types found in the intrauterine environment and fetal respiratory, digestive and external barrier tissues of the fetus, using high-confidence cellular molecular markers. While some RNAs and splice variants were present throughout pregnancy, many transcripts were uniquely expressed at different time points in pregnancy and associated with distinct neonatal co-morbidities (respiratory distress and gavage feeding), indicating fetal immaturity. Conclusion The AF transcriptome exhibits unique cell/organ-selective expression patterns at different time points in pregnancy that can potentially identify fetal organ maturity and predict neonatal morbidity. Developing novel biomarkers indicative of the maturation of multiple organ systems can improve upon our current methods of fetal maturity testing which focus solely on the lung, and will better inform obstetrical decisions regarding delivery timing.
机译:背景羊水(AF)是胎儿的近端液体,比母体血清含有更多的无细胞胎儿RNA / DNA,因此使其成为鉴定预测胎儿发育和器官成熟的新型生物标记物的有希望的来源。我们的目的是比较妊娠不同时间点的AF转录组谱,以证明独特的遗传特征,可作为指示胎儿成熟的潜在生物标记。方法我们从16个孕妇在怀孕的不同时间点分离出AF RNA:18至24周为4个,34至36周为6个,39至40周为6个。 RNA测序是在无细胞RNA上进行的。结合细胞类型和途径预测进行基因表达和剪接分析。结果在妊娠的不同时间点进行的样品水平分析表明,使用高信度细胞分子标记物与子宫内环境以及胎儿的胎儿呼吸道,消化道和外部屏障组织中发现的细胞类型密切相关。尽管在整个怀孕期间都存在一些RNA和剪接变体,但许多转录本在怀孕的不同时间点独特表达,并与不同的新生儿合并症(呼吸窘迫和管饲喂养)有关,表明胎儿不成熟。结论AF转录组在妊娠的不同时间点表现出独特的细胞/器官选择性表达模式,可以潜在地识别胎儿器官成熟并预测新生儿发病率。开发表明多种器官系统成熟的新型生物标志物可以改善我们目前仅以肺为中心的胎儿成熟度测试方法,并将更好地为产科有关分娩时机的决策提供依据。

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