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利用具有随机序列的底物在体外确定HIV-1整合酶与U3和U5末端序列的相互作用。

HIV-1 integrase interaction with U3 and U5 terminal sequences in vitro defined using substrates with random sequences.

作者信息

Brin Elena, Leis Jonathan

机构信息

Department of Microbiology and Immunology, Northwestern University School of Medicine, Chicago, Illinois 60611, USA.

出版信息

J Biol Chem. 2002 May 24;277(21):18357-64. doi: 10.1074/jbc.M201354200. Epub 2002 Mar 15.

DOI:10.1074/jbc.M201354200
PMID:11897790
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2769074/
Abstract

Successful integration of viral genome into a host chromosome depends on interaction between viral integrase and its recognition sequences. We have used a reconstituted concerted human immunodeficiency virus, type 1 (HIV-1), integration system to analyze the role of integrase (IN) recognition sequences in formation of the IN-viral DNA complex capable of concerted integration. HIV-1 integrase was presented with substrates that contained all 4 bases at 8 mismatched positions that define the inverted repeat relationship between U3 and U5 long terminal repeats (LTR) termini and at positions 17-19, which are conserved in the termini. Evidence presented indicates that positions 17-20 of the IN recognition sequences are needed for a concerted DNA integration mechanism. All 4 bases were found at each randomized position in sequenced concerted DNA integrants, although in some instances there were preferences for specific bases. These results indicate that integrase tolerates a significant amount of plasticity as to what constitutes an IN recognition sequence. By having several positions randomized, the concerted integrants were examined for statistically significant relationships between selections of bases at different positions. The results of this analysis show not only relationships between different positions within the same LTR end but also between different positions belonging to opposite DNA termini.

摘要

病毒基因组成功整合到宿主染色体上取决于病毒整合酶与其识别序列之间的相互作用。我们使用了一种重组的1型人类免疫缺陷病毒(HIV-1)协同整合系统,来分析整合酶(IN)识别序列在形成能够进行协同整合的IN-病毒DNA复合物中的作用。给HIV-1整合酶提供的底物在8个错配位置含有所有4种碱基,这些位置定义了U3和U5长末端重复序列(LTR)末端之间的反向重复关系,以及在末端保守的17-19位。所提供的证据表明,IN识别序列的17-20位对于协同DNA整合机制是必需的。在测序的协同DNA整合体中,在每个随机化位置都发现了所有4种碱基,尽管在某些情况下对特定碱基有偏好。这些结果表明,整合酶对于构成IN识别序列的要素具有很大的可塑性。通过使几个位置随机化,对协同整合体进行了分析,以研究不同位置碱基选择之间的统计学显著关系。该分析结果不仅显示了同一LTR末端内不同位置之间的关系,还显示了属于相反DNA末端的不同位置之间的关系。

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本文引用的文献

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Changes in the mechanism of DNA integration in vitro induced by base substitutions in the HIV-1 U5 and U3 terminal sequences.HIV-1 U5和U3末端序列中的碱基替换诱导的体外DNA整合机制变化
J Biol Chem. 2002 Mar 29;277(13):10938-48. doi: 10.1074/jbc.M108116200. Epub 2002 Jan 11.
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