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首页> 外文期刊>International journal of molecular medicine >Expression profile of microRNAs in fetal lung development of Sprague-Dawley rats
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Expression profile of microRNAs in fetal lung development of Sprague-Dawley rats

机译:microRNA在Sprague-Dawley大鼠胎肺发育中的表达谱

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As well-known regulators of gene expression, microRNAs (miRNAs) play an important role not only in cell proliferation and differentiation, but also in tumorigenesis and organ development. Furthermore, it is estimated that miRNAs may be responsible for regulating the expression of nearly one-third of the human genome. Simultaneously, in the clinic, with advances in neonatal care, a larger number of premature infants are being saved, and thus diseases of lung development, including bronchopulmonary dysplasia (BPD) have become more and more common. However, only a few miRNA studies have studied their connection with diseases of lung development. In our study, we used a miRNA microarray including more than 1891 capture probes to profile the expression of miRNAs at three time points of rat lung development [embryonic (E) Day 16 (E16), E19, E21]. miRNAs found to have consistent fold-changes (fold-change>2.0) during all three time points were selected and validated by real-time PCR. As a result, 167 differentially expressed miRNAs were found during rat lung organogenesis, including 81 upregulated and 86 downregulated miRNAs. Seven miRNAs were selected and characterized by having a consistent >2-fold changes between all three groups. Among these 7 miRNAs, except for let-7a, the other 6 miRNAs (miR-1949, miR-125b-5p, miR-296, miR-93, miR-146b, miR-3560) are all first reported for the first time in lung development. Finally, due to the fact that they demonstrated higher fold changes, from these 7 miRNAs we selected miR-125b-5p, miR-296, miR-93, miR-146b and miR-3560 for real-time PCR. We hypothesized that these newly identified miRNAs may play an important role in fetal lung development, and this experimental result could help us to further clarify the mechanism of normal lung development including the development of type?II pneumocytes. This may provide a physiological basis for future research on diseases of lung development.
机译:作为众所周知的基因表达调节剂,微小RNA(miRNA)不仅在细胞增殖和分化中起重要作用,而且在肿瘤发生和器官发育中也起重要作用。此外,据估计,miRNA可能负责调节人类基因组近三分之一的表达。同时,在临床上,随着新生儿护理的进步,越来越多的早产儿得以挽救,因此,包括支气管肺发育不良(BPD)在内的肺部发育疾病变得越来越普遍。但是,只有很少的miRNA研究研究了它们与肺发育疾病的联系。在我们的研究中,我们使用了包括超过1891个捕获探针的miRNA微阵列,以在大鼠肺发育的三个时间点分析miRNA的表达[胚胎(E)第16天(E16),E19,E21]。选择了在所有三个时间点均具有一致的倍数变化(倍数变化> 2.0)的miRNA,并通过实时PCR进行了验证。结果,在大鼠肺器官发生过程中发现了167个差异表达的miRNA,包括81个上调的miRNA和86个下调的miRNA。选择了七个miRNA,并通过在所有三组之间的一致> 2倍变化来表征。在这7个miRNA中,除了let-7a之外,其他6个miRNA(miR-1949,miR-125b-5p,miR-296,miR-93,miR-146b,miR-3560)都是首次首次报道。在肺部发育。最后,由于它们表现出更高的倍数变化,我们从这7个miRNA中选择了miR-125b-5p,miR-296,miR-93,miR-146b和miR-3560进行实时PCR。我们假设这些新鉴定的miRNA在胎儿肺发育中可能起重要作用,并且该实验结果可以帮助我们进一步阐明正常肺发育的机制,包括II型肺细胞的发育。这可能为将来的肺部发育疾病研究提供生理基础。

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