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不同序列相似性对1型人类免疫缺陷病毒载体逆转录过程中重复序列缺失频率的影响。

Effects of varying sequence similarity on the frequency of repeat deletion during reverse transcription of a human immunodeficiency virus type 1 vector.

作者信息

An Wenfeng, Telesnitsky Alice

机构信息

Department of Microbiology and Immunology, University of Michigan Medical School, Ann Arbor, Michigan 48109-0620, USA.

出版信息

J Virol. 2002 Aug;76(15):7897-902. doi: 10.1128/jvi.76.15.7897-7902.2002.

DOI:10.1128/jvi.76.15.7897-7902.2002
PMID:12097604
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC136404/
Abstract

Genetic recombination contributes to human immunodeficiency virus type 1 (HIV-1) diversity, with homologous recombination being more frequent than nonhomologous recombination. In this study, HIV-1-based vectors were used to assay the effects of various extents of sequence divergence on the frequency of the recombination-related property of repeat deletion. Sequence variation, similar in degree to that which differentiates natural HIV-1 isolates, was introduced by synonymous substitutions into a gene segment. Repeated copies of this segment were then introduced into assay vectors. With the use of a phenotypic screen, the deletion frequency of identical repeats was compared to the frequencies of repeats that differed in sequence by various extents. During HIV-1 reverse transcription, the deletion frequency observed with repeats that differed by 5% was 65% of that observed with identical repeats. The deletion frequency decreased to 26% for repeats that differed by 9%, and when repeats differed by 18%, the deletion frequency was about 5% of the identical repeat value. Deletion frequencies fell to less than 0.3% of identical repeat values when genetic distances of 27% or more were examined. These data argue that genetic variation is not as inhibitory to HIV-1 repeat deletion as it is to the corresponding cellular process and suggest that, for sequences that differ by about 25% or more, HIV-1 recombination directed by sequence homology may be no more frequent than that which is homology independent.

摘要

基因重组有助于人类免疫缺陷病毒1型(HIV-1)的多样性,其中同源重组比非同源重组更为频繁。在本研究中,基于HIV-1的载体被用于检测不同程度的序列差异对重复序列缺失这一重组相关特性频率的影响。通过同义替换将与区分天然HIV-1分离株程度相似的序列变异引入一个基因片段。然后将该片段的重复拷贝引入检测载体。通过表型筛选,将相同重复序列的缺失频率与序列存在不同程度差异的重复序列的频率进行比较。在HIV-1逆转录过程中,序列差异为5%的重复序列的缺失频率是相同重复序列缺失频率的65%。序列差异为9%的重复序列的缺失频率降至26%,当重复序列差异为18%时,缺失频率约为相同重复序列值的5%。当检测到27%或更高的遗传距离时,缺失频率降至相同重复序列值的0.3%以下。这些数据表明,基因变异对HIV-1重复序列缺失的抑制作用不如对相应细胞过程的抑制作用,并且表明,对于差异约为25%或更大的序列,由序列同源性指导的HIV-1重组可能并不比非同源重组更频繁。

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本文引用的文献

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Dynamic copy choice: steady state between murine leukemia virus polymerase and polymerase-dependent RNase H activity determines frequency of in vivo template switching.动态拷贝选择:小鼠白血病病毒聚合酶与聚合酶依赖性核糖核酸酶H活性之间的稳态决定体内模板转换频率。
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