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Hepatitis B viral DNA is methylated in liver tissues.

机译:乙肝病毒DNA在肝组织中甲基化。

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摘要

The mechanisms that regulate hepatitis B virus (HBV) replication within the liver are poorly understood. Given that methylation of CpG islands regulates gene expression in human tissues, we sought to identify CpG islands in HBV-DNA and to determine if they are methylated in human tissues. In silico analysis demonstrated three CpG islands in HBV genotype A sequences, two of which were of particular interest because of their proximity to the HBV surface gene start codon (island 1) and to the enhancer 1/X gene promoter region (island 2). Human sera with intact virions that were largely unmethylated were used to transfect HepG2 cells and HBV-DNA became partially methylated at both islands 1 and 2 by day 6 following exposure of HepG2 to virus. Examination of three additional human sera and 10 liver tissues showed no methylation in sera but tissues showed methylation of island 1 in six of 10 cases and of island 2 in five of 10 cases. The cell line Hep3B, with integrated HBV, showed complete methylation of island 1 but no methylation of island 2. In conclusion, HBV-DNA can be methylated in human tissues and methylation may play an important role in regulation of HBV gene expression.
机译:对肝脏中调节乙型肝炎病毒(HBV)复制的机制了解甚少。鉴于CpG岛的甲基化调节人体组织中的基因表达,我们试图鉴定HBV-DNA中的CpG岛,并确定它们是否在人体组织中被甲基化。在计算机分析中证实了HBV基因型A序列中的三个CpG岛,其中两个特别重要,因为它们靠近HBV表面基因起始密码子(岛1)和增强子1 / X基因启动子区(岛2)。具有完整未完全甲基化的完整病毒体的人血清被用于转染HepG2细胞,并且在HepG2暴露于病毒后第6天,HBV-DNA在岛1和岛2均被部分甲基化。对另外三个人血清和十个肝组织的检查显示,血清中无甲基化,但组织显示十个病例中有六个的岛1和十个例子中有五个的岛2甲基化。具有整合的HBV的Hep3B细胞系显示岛1完全甲基化,但岛2没有甲基化。总而言之,HBV-DNA在人体组织中可以被甲基化,甲基化可能在调节HBV基因表达中起重要作用。

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