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首页> 外文期刊>International Journal of Cancer =: Journal International du Cancer >Genome-wide small nucleolar RNA expression analysis of lung cancer by next-generation deep sequencing
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Genome-wide small nucleolar RNA expression analysis of lung cancer by next-generation deep sequencing

机译:下一代深度测序分析肺癌的全基因组小核仁RNA表达

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摘要

Emerging evidence indicates that small nucleolar RNAs (snoRNAs), a class of small noncoding RNAs, may play important function in tumorigenesis. Nonsmall-cell lung cancer (NSCLC) is the number one cancer killer for men and women. Systematically characterizing snoRNAs in NSCLC will develop biomarkers for its early detection and prognostication. We used next-generation deep sequencing to comprehensively characterize snoRNA profiles in 12 NSCLC tissues. We used quantitative reverse transcription polymerase chain reaction (qRT-PCR) to verify the findings in 40 surgical Stage I NSCLC specimens and 126 frozen NSCLC tissues of different stages. The 126 NSCLC tissues were divided into a training set and a testing set. Deep sequencing identified 458 snoRNAs, of which, 29 had a 3.0-fold expression level change in Stage I NSCLC tissues versus normal tissues. qRT-PCR analysis showed that 16 of 29 snoRNAs exhibited consistent changes with deep sequencing data. The 16 snoRNAs exhibited 0.75-0.94 area under receiver-operator characteristic curve values in distinguishing lung tumor from normal lung tissues (all 0.0001) with 70.0-95.0% sensitivity and 70.0-95.0% specificity. Six genes (snoRA47, snoRA68, snoRA78, snoRA21, snoRD28 and snoRD66) were identified whose expressions were associated with overall survival of the NSCLC patients. A prediction model consisting of three genes (snoRA47, snoRA68 and snoRA78) was developed in the training set of 77 cases, which could significantly predict overall survival of the NSCLC patients (p<0.0001). The prognostic performance of the prediction model was confirmed in the testing set of 49 NSCLC patients. The identified snoRNA signatures may provide potential biomarkers for the early detection and prognostication of NSCLC.
机译:新兴证据表明,小的核仁RNA(snoRNA)是一类小的非编码RNA,可能在肿瘤发生中起重要作用。非小细胞肺癌(NSCLC)是男性和女性的头号杀手。在NSCLC中系统表征snoRNA将为早期检测和预后开发生物标志物。我们使用了下一代深度测序技术来全面表征12种NSCLC组织中的snoRNA配置文件。我们使用定量逆转录聚合酶链反应(qRT-PCR)验证了40例手术I期非小细胞肺癌标本和126个不同阶段的冷冻NSCLC组织中的发现。将126个NSCLC组织分为训练组和测试组。深度测序鉴定出458种snoRNA,其中29种在I期非小细胞肺癌组织中的表达水平是正常组织的3.0倍。 qRT-PCR分析显示,29种snoRNA中有16种在深度测序数据方面表现出一致的变化。在区分肺癌和正常肺组织(均为0.0001)时,这16种snoRNA在接收者-操作者特征曲线值下显示0.75-0.94面积,具有70.0-95.0%的敏感性和70.0-95.0%的特异性。鉴定了六个基因(snoRA47,snoRA68,snoRA78,snoRA21,snoRD28和snoRD66),其表达与NSCLC患者的整体存活率相关。在77例患者的训练集中建立了由三个基因(snoRA47,snoRA68和snoRA78)组成的预测模型,该模型可以显着预测NSCLC患者的总体生存率(p <0.0001)。在49例NSCLC患者的测试集中证实了预测模型的预后性能。鉴定出的snoRNA标记可能为NSCLC的早期检测和预后提供潜在的生物标记。

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