首页> 外文期刊>International Journal of Cancer =: Journal International du Cancer >Genome-wide small noncoding RNA profiling of pediatric high-grade gliomas reveals deregulation of several miRNAs, identifies downregulation of snoRNA cluster HBII-52 and delineates H3F3A and TP53 mutant-specific miRNAs and snoRNAs
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Genome-wide small noncoding RNA profiling of pediatric high-grade gliomas reveals deregulation of several miRNAs, identifies downregulation of snoRNA cluster HBII-52 and delineates H3F3A and TP53 mutant-specific miRNAs and snoRNAs

机译:儿科高级神经胶质瘤的全基因组小非编码RNA分析揭示了几种miRNA的失调,鉴定了snoRNA簇HBII-52的下调并描绘了H3F3A和TP53突变体特异的miRNA和snoRNA

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Pediatric high-grade gliomas (HGGs) are highly malignant tumors that remain incurable and relatively understudied. The crucial role of noncoding RNAs (ncRNAs) has been reported in various cancers. However, the study on miRNAs in pediatric HGGs is scant and there is no report till date on the status of other small ncRNAs. Genome-wide microarray analysis was performed to investigate small ncRNA expression in pediatric HGG (n=14) and compared to adult glioblastoma (GBM) signature. The validation of miRNAs and small nucleolar RNAs (snoRNAs) was done by real-time polymerase chain reaction. TP53 and H3F3A mutation-specific miRNA and snoRNA profiles were generated and analyzed. Pediatric HGGs showed upregulation of miR-17/92 and its paralog clusters (miR106b/25 and miR106a/363), whereas majority of downregulated miRNAs belonged to miR379/656 cluster (14q32). Unsupervised hierarchical clustering identified two distinct groups. Interestingly, Group 2 with downregulated 14q32 cluster showed better overall survival. The miRNAs unique to pediatric HGG as compared to adult GBM were predicted to affect PDGFR and SMAD2/3 pathways. Similarities were seen between pediatric HGG and TP53 mutant miRNA profiles as compared to wild types. Several of H3F3A mutation-regulated genes were found to be the targets of H3F3A mutant-specific miRNAs. Remarkably, a significant downregulation of HBII-52 snoRNA cluster was found in pediatric HGGs, and was specific to H3F3A nonmutants. This is the first genome-wide profiling study on miRNAs and snoRNAs in pediatric HGGs with respect to H3F3A and TP53 mutations. The comparison of miRNA profiles of pediatric HGGs and adult GBM reiterates the overlaps and differences as also seen with their gene expression and methylation signatures.
机译:儿科高级别神经胶质瘤(HGG)是高度恶性的肿瘤,仍无法治愈且研究相对较少。非编码RNA(ncRNA)的关键作用已在各种癌症中报道。但是,关于小儿HGGs中miRNA的研究很少,迄今为止尚无其他小ncRNA的状态的报道。进行了全基因组微阵列分析,以调查小儿HGG(n = 14)中的小ncRNA表达,并将其与成年胶质母细胞瘤(GBM)签名进行比较。 miRNA和小核仁RNA(snoRNA)的验证是通过实时聚合酶链反应完成的。生成并分析了TP53和H3F3A突变特异性miRNA和snoRNA图谱。小儿HGGs显示miR-17 / 92及其旁系簇(miR106b / 25和miR106a / 363)上调,而大多数下调的miRNA属于miR379 / 656簇(14q32)。无监督的层次聚类确定了两个不同的组。有趣的是,第2q组的14q32簇被下调显示出更好的总体存活率。与成人GBM相比,小儿HGG特有的miRNA预计会影响PDGFR和SMAD2 / 3途径。与野生型相比,小儿HGG和TP53突变体miRNA图谱之间存在相似性。发现一些H3F3A突变调控基因是H3F3A突变体特异性miRNA的靶标。值得注意的是,在儿科HGG中发现HBII-52 snoRNA簇明显下调,并且对H3F3A非突变体具有特异性。这是关于H3F3A和TP53突变的小儿HGG中miRNA和snoRNA的首次全基因组分析。儿科HGGs和成人GBM的miRNA图谱的比较重申了它们的重叠和差异,以及它们的基因表达和甲基化特征。

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