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HIV-1 DIS stem loop forms an obligatory bent kissing intermediate in the dimerization pathway

机译:HIV-1 DIS阀圈环形在二聚化途径中形成义务弯曲接吻中间体

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摘要

The HIV-1 dimerization initiation sequence (DIS) is a conserved palindrome in the apical loop of a conserved hairpin motif in the 5'-untranslated region of its RNA genome. DIS hairpin plays an important role in genome dimerization by forming a 'kissing complex' between two complementary hairpins. Understanding the kinetics of this interaction is key to exploiting DIS as a possible human immunodeficiency virus (HIV) drug target. Here, we present a single-molecule Forster resonance energy transfer (smFRET) study of the dimerization reaction kinetics. Our data show the real-time formation and dissociation dynamics of individual kissing complexes, as well as the formation of the mature extended duplex complex that is ultimately required for virion packaging. Interestingly, the single-molecule trajectories reveal the presence of a previously unobserved bent intermediate required for extended duplex formation. The universally conserved A272 is essential for the formation of this intermediate, which is stabilized by Mg2+, but not by K+ cations. We propose a 3D model of a possible bent intermediate and a minimal dimerization pathway consisting of three steps with two obligatory intermediates (kissing complex and bent intermediate) and driven by Mg2+ ions
机译:HIV-1二聚化起始序列(DIS)是在其RNA基因组的5'-未翻译区域中的保守发夹基序的顶端环路中的保守回路。 DIS发夹通过在两个互补发夹之间形成“亲吻复合物”来在基因组二聚体中起重要作用。理解这种相互作用的动力学是利用DIS作为可能的人类免疫缺陷病毒(HIV)药物靶标的关键。这里,我们介绍了二聚反应动力学的单分子福斯特共振能量转移(SMFRet)研究。我们的数据显示了个体接吻复合物的实时形成和解离动力,以及成熟的扩展双工复合体的形成最终需要进行病毒赛衣物。有趣的是,单分子轨迹揭示了延长双链体形成所需先前未被检测的弯曲中间的存在。普遍保守的A272对于形成这种中间体至关重要,该中间体由Mg2 +稳定,但不是K +阳离子稳定。我们提出了一种可能的弯曲中间体的3D模型和由具有两个强制中间体(接吻复合物和弯曲中间体)的三个步骤组成的最小二聚化途径,并由Mg2 +离子驱动

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  • 来源
    《Nucleic Acids Research》 |2014年第11期|共9页
  • 作者单位

    Department of Chemistry Wayne State University Detroit MI 48236 USA;

    Department of Chemistry Wayne State University Detroit MI 48236 USA;

    Department of Chemistry Wayne State University Detroit MI 48236 USA;

    Architecture et Réactivité de l'ARN Université de Strasbourg Institut de Biologie Moléculaire et Cellulaire du CNRS F-67084 Strasbourg France;

    Department of Chemistry Wayne State University Detroit MI 48236 USA;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 生物化学;
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