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Human hepatocellular carcinoma cell-specific miRNAs reveal the differential expression of miR-24 and miR-27a in cirrhoticon-cirrhotic HCC

机译:人类肝癌细胞特异的miRNA显示肝硬化/非肝硬化HCC中miR-24和miR-27a的差异表达

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摘要

microRNAs (miRs) are 18–25 nucleotide non-coding RNAs that regulate gene expression in several physiological and pathological conditions. To gather more knowledge on microRNAs in human hepatocellular carcinoma (HCC) we generated a small RNA library in the human HCC cell line HA22T/VGH by cloning and sequencing the cDNA obtained following the size selection of 18–24 nucleotide RNAs. We determined the expression levels of the most frequently cloned microRNAs by qPCR in HCC tissues and in their peritumoral counterparts from biopsy specimens of 41 HCC patients. The most frequently cloned miRs were miR-24, miR-27a and miR-21, and their expression levels in human HCC tissues indicate that these miRs were dysregulated in HCC. We showed that miR-24 and miR-27a were significantly downregulated in HCCs from cirrhotic liver tissues in comparison to those from non-cirrhotic liver tissues. In cirrhotic HCCs the downregulation of miR-24 was correlated with poorer prognosis in patients with HBV and HCV virus infections. miR-21 was generally upregulated in HCC tissues versus the corresponding peritu-moral tissues, particularly in non-cirrhotic HCC. Furthermore, by sequence alignment we identified the human miR orthologue of Mus musculus miR-1199 not yet annotated. Our results outline the differential expression of miRs in cirrhotic and non-cirrhotic HCCs, thereby contributing to advances in the discovery and validation of novel molecular biomarkers of HCC progression.
机译:microRNA(miR)是18-25个核苷酸的非编码RNA,可在几种生理和病理条件下调节基因表达。为了收集有关人类肝细胞癌(HCC)中microRNA的更多知识,我们通过克隆和测序18–24个核苷酸RNA的大小选择后获得的cDNA,在人类HCC细胞系HA22T / VGH中生成了一个小的RNA文库。我们通过qPCR测定了41例HCC患者活检样本中HCC组织及其癌旁对应物中最常克隆的microRNA的表达水平。克隆最频繁的miR是miR-24,miR-27a和miR-21,它们在人HCC组织中的表达水平表明这些miR在HCC中表达失调。我们显示,与非肝硬化肝组织相比,肝硬化肝组织的HCC中miR-24和miR-27a显着下调。在肝硬化性肝癌中,miR-24的下调与HBV和HCV病毒感染患者的预后较差有关。与肝癌组织相比,在肝癌组织中miR-21通常上调,尤其是在非肝硬化性肝癌中。此外,通过序列比对,我们鉴定了尚未注释的小家鼠miR-1199的人miR直系同源物。我们的研究结果概述了肝硬化和非肝硬化肝癌中miRs的差异表达,从而有助于发现和验证新型肝癌进展分子生物学标志物。

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