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一种不同寻常的自我引发逆转录机制需要逆转录酶的核糖核酸酶H结构域切割RNA双链体。

An unusual mechanism of self-primed reverse transcription requires the RNase H domain of reverse transcriptase to cleave an RNA duplex.

作者信息

Levin H L

机构信息

Laboratory of Eukaryotic Gene Regulation, National Institute of Child Health and Human Development, Bethesda, Maryland 20892, USA.

出版信息

Mol Cell Biol. 1996 Oct;16(10):5645-54. doi: 10.1128/MCB.16.10.5645.

Abstract

The reverse transcription of retroviruses and long terminal repeat-containing retrotransposons requires that tRNA species serve as primers. We recently reported that the long terminal repeat-containing retrotransposon Tf1 is a unique exception in that reverse transcription is independent of tRNA and is instead initiated by a self-priming mechanism. The first 11 bases of the Tf1 transcript fold back and anneal to the primer binding site in a process that results in the priming of minus-strand strong-stop DNA. Data presented here demonstrate that a cleavage occurs between the 11th and 12th bases of the transcript, resulting in the generation of the primer. Mutagenesis experiments presented here indicate that the RNase H domain of the Tf1 reverse transcriptase is required for the cleavage reaction, suggesting that this RNase H may have the novel ability to cleave double-stranded RNA at the end of a duplexed region.

摘要

逆转录病毒和含长末端重复序列的逆转座子的逆转录需要特定的tRNA作为引物。我们最近报道,含长末端重复序列的逆转座子Tf1是一个独特的例外,其逆转录不依赖tRNA,而是通过一种自我引发机制启动。Tf1转录本的前11个碱基回折并与引物结合位点退火,这一过程导致负链强终止DNA的引发。此处呈现的数据表明,转录本的第11和12个碱基之间发生了切割,从而产生了引物。此处进行的诱变实验表明,Tf1逆转录酶的RNase H结构域是切割反应所必需的,这表明这种RNase H可能具有在双链区域末端切割双链RNA的新能力。

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