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Hepatitis B virus integration in hepatocellular carcinoma DNA: duplication of cellular flanking sequences at the integration site.

机译:乙型肝炎病毒在肝细胞癌DNA中的整合:在整合位点的细胞侧翼序列重复。

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摘要

The integrated form of hepatitis B virus (HBV) in the human hepatoma cell line huH2-2 and its cellular counterpart sequence have been cloned and analyzed. Blot hybridization analysis and nucleotide sequencing indicated that a single copy of the 1895-base-pair (bp) subgenomic region of HBV DNA, spanning from the middle of pre-S to the end of gene X, was integrated and flanked by the 12-bp directly repeating cellular sequences. A comparison of the sequencing data with that of the cellular counterpart DNA indicated the absence of deletion and rearrangement in the cellular flanking DNA following integration of the 1895-bp HBV DNA, except for generation of the 12-bp direct repeat at the virus-cell junction. A possible model for the mechanism of HBV integration is proposed.
机译:已克隆和分析了人类肝癌细胞系huH2-2中乙型肝炎病毒(HBV)的整合形式及其细胞对应序列。印迹杂交分析和核苷酸测序表明,HBV DNA的1895个碱基对(bp)亚基因组区域的单个副本(从pre-S的中间到基因X的末端)被整合并位于12- bp直接重复细胞序列。测序数据与细胞对应DNA的比较表明,整合了1895-bp HBV DNA后,细胞侧翼DNA中没有缺失和重排,除了在病毒细胞中产生了12-bp直接重复之外交界处。提出了HBV整合机制的可能模型。

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