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Template Switches during Plus-Strand DNA Synthesis of Duck Hepatitis B Virus Are Influenced by the Base Composition of the Minus-Strand Terminal Redundancy

机译:鸭乙型肝炎病毒正链DNA合成过程中的模板转换受负链末端冗余的碱基组成的影响

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摘要

Two template switches are necessary during plus-strand DNA synthesis of the relaxed circular (RC) form of the hepadnavirus genome. The 3′ end of the minus-strand DNA makes important contributions to both of these template switches. It acts as the donor site for the first template switch, called primer translocation, and subsequently acts as the acceptor site for the second template switch, termed circularization. Circularization involves transfer of the nascent 3′ end of the plus strand from the 5′ end of the minus-strand DNA to the 3′ end, where further elongation can lead to production of RC DNA. In duck hepatitis B virus (DHBV), a small terminal redundancy (5′r and 3′r) on the ends of the minus-strand DNA has been shown to be important, but not sufficient, for circularization. We investigated what contribution, if any, the base composition of the terminal redundancy made to the circularization process. Using a genetic approach, we found a strong positive correlation between the fraction of A and T residues within the terminal redundancy and the efficiency of the circularization process in those variants. Additionally, we found that the level of in situ priming increases, at the expense of primer translocation, as the fraction of A and T residues in the 3′r decreases. Thus, a terminal redundancy rich in A and T residues is important for both plus-strand template switches in DHBV.
机译:在肝炎病毒基因组的松弛环状(RC)形式的正链DNA合成过程中,需要两个模板开关。负链DNA的3'端对这两个模板开关都做出了重要贡献。它充当第一个模板开关的供体位点,称为引物易位,随后充当第二个模板开关的受体位点,称为环化。环化涉及将正链的新生3'末端从负链DNA的5'末端转移到3'末端,在此处进一步延伸可导致产生RC DNA。在鸭乙型肝炎病毒(DHBV)中,负链DNA末端的小末端冗余(5'r和3'r)已显示对环化很重要,但不足。我们研究了终端冗余对环化过程的基础组成(如果有)的贡献。使用遗传方法,我们发现末端冗余中A和T残基的比例与这些变体中环化过程的效率之间存在很强的正相关性。此外,我们发现,随着3'r中A和T残基的比例降低,原位引发的水平增加,但引物易位损失。因此,对于DHBV中的两个正链模板开关,富含A和T残基的末端冗余非常重要。

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