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Identification of latent biomarkers in hepatocellular carcinoma by ultra-deep whole-transcriptome sequencing

机译:超深度全转录组测序鉴定肝细胞癌潜在生物标志物

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摘要

There is an urgent need to identify biomarkers for hepatocellular carcinoma due to limited treatment options and the poor prognosis of this common lethal disease. Whole-transcriptome shotgun sequencing (RNA-Seq) provides new possibilities for biomarker identification. We sequenced 鈭?/span>250 million pair-end reads from a pair of adjacent normal and tumor liver samples. With the aid of bioinformatics tools, we determined the transcriptome landscape and sought novel biomarkers by further empirical validations in 55 pairs of adjacent normal and tumor liver samples with various viral statuses such as HBV(+), HCV(+) and HBV(鈭?HCV(鈭?. We identified a novel gene with coding regions, termed DUNQU1 , which has a tissue-specific expression pattern in tumor liver samples of HCV(+) and HBV(鈭?HCV(鈭? hepatocellular carcinomas. Overexpression of DUNQU1 in Huh7 cell lines enhances the ability to form colonies in soft agar. Also, we identified three novel differentially-expressed protein-coding genes (ALG1L , SERPINA11 and TMEM82 ) that lack documented expression profiles in liver cancer and showed that the level of SREPINA11 is correlated with pathology stages. Moreover, we showed that the alternative splicing event of FGFR2 is associated with virus infection, tumor size, cirrhosis and tumor recurrence. The findings indicate that these new markers of hepatocellular carcinoma may be of value in improving prognosis and could have potential as new targets for developing new treatment options.
机译:由于有限的治疗选择和这种常见致死性疾病的不良预后,迫切需要鉴定肝细胞癌的生物标志物。全转录组shot弹枪测序(RNA-Seq)为生物标志物鉴定提供了新的可能性。我们从一对相邻的正常和肿瘤肝脏样品中测序了2.5亿对双末端读数。借助于生物信息学工具,我们通过进一步的经验验证,在55对相邻的正常和肿瘤肝样品中,对各种病毒状态如HBV(+),HCV(+)和HBV(鈭?)进行了实验验证,确定了转录组的格局并寻找了新的生物标记。 HCV(?)。我们鉴定了一个具有编码区的新基因,称为 DUNQU1,该基因在HCV(+)和HBV(?HCV(?)肝细胞癌的肿瘤肝样品中具有组织特异性表达模式。 Huh7细胞系中 DUNQU1的表达增强了在软琼脂中形成菌落的能力。此外,我们鉴定了三个新的差异表达的蛋白质编码基因( ALG1L, SERPINA11和 TMEM82)文献报道了肝癌中的表达谱,表明 SREPINA11的水平与病理分期有关,而且,我们表明 FGFR2的可变剪接事件与病毒感染,肿瘤大小,肝硬化和肿瘤复发有关。调查结果表明,这些新市场肝细胞癌可能在改善预后方面具有价值,并有可能作为开发新治疗方案的新靶标。

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