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Variations in gene expression and genomic stability of human hepatoma cells integrated with hepatitis B virus DNA

机译:乙型肝炎病毒DNA整合的人肝癌细胞的基因表达和基因组稳定性的变化

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The association of hepatitis B virus (HBV) infection with human hepatoma is well established. However, no consensus regarding the etiology of hepatocellular carcinoma was elucidated. In this paper, the genomic stability and gene expression of HBV DNA-integrated and non-integrated hepatoma cells by Transcript Profile (TP)-PCR and RT-PCR are characterized. The additional DNA bands generated from TP-PCR of HBV integrated genomes were not correlated with the sequence of HBV, suggesting that the variations may result from genomic instability of the host cells. Moreover, differential genes expressed in HBV DNA-integrated cells were sequenced. A cDNA generated from the integrated cells exhibited 99.3% homology with the sequences of ATP synthase 6 and cytochrome C oxidase III, but the sequences were abnormally linked together. Since HBV infection may alter the energy metabolism of the cell, the results suggest that the integration may cause mitochondriae defects in the ATP synthase 6 and cytochrome C oxidase III genes.
机译:乙型肝炎病毒(HBV)感染与人肝癌之间的关联已得到充分证实。但是,尚无关于肝细胞癌病因的共识。本文通过转录本(TP)-PCR和RT-PCR对HBV DNA整合的和非整合的肝癌细胞的基因组稳定性和基因表达进行了表征。从HBV整合基因组的TP-PCR产生的其他DNA条带与HBV序列不相关,这表明变异可能是由于宿主细胞的基因组不稳定性所致。此外,对在HBV DNA整合细胞中表达的差异基因进行了测序。由整合细胞产生的cDNA与ATP合酶6和细胞色素C氧化酶III的序列具有99.3%的同源性,但是这些序列被异常地连接在一起。由于HBV感染可能会改变细胞的能量代谢,因此结果表明整合可能会导致ATP合酶6和细胞色素C氧化酶III基因中的线粒体缺陷。

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