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Genomic modeling of hepatitis B virus integration frequency in the human genome

机译:人类基因组中乙型肝炎病毒整合频率的基因组建模

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摘要

Hepatitis B infection is a world-wide public health burden causing serious liver complications. Previous studies suggest that hepatitis B integration into the human genome plays a crucial role in triggering oncogenic process and may also constitutively produce viral antigens. Despite the progress in HBV biology and sequencing technology, our fundamental understanding of how many hepatocytes in the liver actually carry viral integrations is still lacking. Herein we provide evidence that the HBV virus integrates with a lower-bound frequency of 0.84 per diploid genome in hepatitis B positive hepatocellular cancer patients. Moreover, we calculate that integrated viral DNA generates ~80% of the HBsAg transcripts in these patients. These results underscore the need to re-evaluate the clinical end-point and treatment strategies for chronic hepatitis B patients.
机译:乙型肝炎感染是导致严重肝并发症的全球性公共卫生负担。先前的研究表明,乙型肝炎整合到人类基因组中在触发致癌过程中起着至关重要的作用,并且还可能组成性地产生病毒抗原。尽管HBV生物学和测序技术取得了进步,但我们仍然缺乏对肝脏中实际上携带病毒整合的肝细胞数量的基本了解。本文提供的证据表明,在乙型肝炎阳性的肝细胞癌患者中,HBV病毒与每个二倍体基因组的下限频率为0.84整合。此外,我们计算出,在这些患者中,整合的病毒DNA产生了约80%的HBsAg转录本。这些结果强调了需要重新评估慢性乙型肝炎患者的临床终点和治疗策略。

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