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人类免疫缺陷病毒1型核衣壳蛋白与病毒DNA之间的相互作用可能在病毒生命周期中具有重要功能。

Interactions between HIV-1 nucleocapsid protein and viral DNA may have important functions in the viral life cycle.

作者信息

Lapadat-Tapolsky M, De Rocquigny H, Van Gent D, Roques B, Plasterk R, Darlix J L

机构信息

LaboRetro INSERM, Ecole Normale Supérieure de Lyon, France.

出版信息

Nucleic Acids Res. 1993 Feb 25;21(4):831-9. doi: 10.1093/nar/21.4.831.

Abstract

In the virion core of retroviruses, the genomic RNA is tightly associated with nucleocapsid (NC) protein molecules, forming the nucleocapsid structure. NC protein, a highly basic protein with two zinc fingers, is indispensable for RNA dimerization, encapsidation and the initiation of reverse transcription in avian, murine and human retroviruses. Here we show that NC protein of HIV-1 (NCp7) and NCp7 mutants bind to DNA fragments representing proviral DNA sequences, forming stable complexes. NCp7 and NCp7 mutants form high molecular weight complexes with large DNA fragments and show cooperativity in binding to the DNAs. It appears that the conserved basic residues, and not the zinc fingers, are important for complex formation. In addition, NCp7 and several NCp7 mutants protect DNAs from nuclease digestion while the DNA ends appear to be poorly protected. NCp7 has been found to bind to strong stop cDNA, the initial product of reverse transcription, and to promote the annealing of this cDNA to HIV-1 RNA corresponding to the 3' end of the genome. In addition, NCp7 slightly stimulates an in vitro IN cleavage assay. These results indicate that the interactions between NCp7 and proviral DNA may be important during provirus synthesis and/or prior to integration.

摘要

在逆转录病毒的病毒粒子核心中,基因组RNA与核衣壳(NC)蛋白分子紧密结合,形成核衣壳结构。NC蛋白是一种具有两个锌指结构的高度碱性蛋白,对于禽类、鼠类和人类逆转录病毒中的RNA二聚化、包装以及逆转录的起始不可或缺。在此我们表明,HIV-1的NC蛋白(NCp7)和NCp7突变体与代表前病毒DNA序列的DNA片段结合,形成稳定的复合物。NCp7和NCp7突变体与大的DNA片段形成高分子量复合物,并在与DNA的结合中表现出协同性。看来保守的碱性残基而非锌指结构对于复合物的形成很重要。此外,NCp7和几个NCp7突变体可保护DNA不被核酸酶消化,而DNA末端似乎保护不佳。已发现NCp7可与强终止cDNA(逆转录的初始产物)结合,并促进该cDNA与对应于基因组3'端的HIV-1 RNA退火。此外,NCp7对体外整合酶切割试验有轻微刺激作用。这些结果表明,在原病毒合成期间和/或整合之前,NCp7与前病毒DNA之间的相互作用可能很重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c3be/309214/10f4b97d0ee9/nar00053-0056-a.jpg

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