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miRNA profiling identifies deregulated miRNAs associated with osteosarcoma development and time to metastasis in two large cohorts

机译:miRNA分析在两个大型队列中鉴定出与骨肉瘤发育和转移时间相关的失控的miRNA

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摘要

Osteosarcoma (OS) is an aggressive bone tumor primarily affecting children and adolescents. The etiology of OS is not fully understood. Thus, there is a great need to obtain a better understanding of OS development and progression. Alterations in miRNA expression contribute to the required molecular alterations for neoplastic initiation and progression. This study is the first to investigate miRNA expression in OS in a large discovery and validation cohort comprising a total of 101 OS samples. We established the signature of altered miRNA expression in OS by profiling the expression level of 752 miRNAs in 23 OS samples using sensitive LNA‐enhanced qPCR assays. The identified miRNA expression changes were correlated with gene expression in the same samples. Furthermore, miRNA expression changes were validated in a second independent cohort consisting of 78 OS samples. Analysis of 752 miRNAs in the discovery cohort led to the identification of 33 deregulated miRNAs in OS. Twenty‐nine miRNAs were validated with statistical significance in the second cohort comprising 78 OS samples. miRNA/mRNA targets were determined, and 361 genes with an inverse expression of the target miRNA were identified. Both the miRNAs and the identified target genes were associated with multiple pathways related to cancer as well as bone cell biology, thereby correlating the deregulated miRNAs with OS tumorigenesis. An analysis of the prognostic value of the 29 miRNAs identified miR‐221/miR‐222 to be significantly associated with time to metastasis in both cohorts. This study contributes to a more profound understanding of OS tumorigenesis, by substantiating the importance of miRNA deregulation. We have identified and validated 29 deregulated miRNAs in the – to our knowledge – largest discovery and validation cohorts used so far for miRNA analyses in OS. Two of the miRNAs showed a promising potential as prognostic biomarkers for the aggressiveness of OS.
机译:骨肉瘤(OS)是一种侵袭性骨肿瘤,主要影响儿童和青少年。尚未完全了解OS的病因。因此,非常需要更好地了解OS的发展和进步。 miRNA表达的改变有助于肿瘤发生和发展所需的分子改变。这项研究是首次在包含101个OS样本的大型发现和验证队列中研究miRNA在OS中的表达。通过使用敏感的LNA增强qPCR分析对23个OS样品中752个miRNA的表达水平进行分析,我们确定了OS中miRNA表达改变的特征。鉴定出的miRNA表达变化与相同样品中的基因表达相关。此外,在由78个OS样品组成的第二个独立队列中验证了miRNA表达的变化。分析发现队列中的752个miRNA导致鉴定出OS中33个失控的miRNA。在包含78个OS样本的第二个队列中,验证了29个miRNA具有统计学意义。确定了miRNA / mRNA靶标,并鉴定了与靶标miRNA反向表达的361个基因。 miRNA和已鉴定的靶基因均与与癌症以及骨细胞生物学相关的多种途径相关,从而使失调的miRNA与OS肿瘤发生相关。对这29个miRNA的预后价值进行分析后,发现miR‐221 / miR‐222与两组的转移时间均显着相关。这项研究通过证实miRNA解除调控的重要性,有助于对OS肿瘤发生有更深刻的了解。据我们所知,我们已经确定并验证了29种去调控的miRNA,这是迄今为止用于OS中miRNA分析的最大的发现和验证队列。两个miRNA作为OS侵袭性的预后生物标志物显示出有希望的潜力。

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