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蛋白质-RNA 亲吻发夹界面的图谱绘制:Rom 与 Tar-Tar*

Mapping of a protein-RNA kissing hairpin interface: Rom and Tar-Tar*.

作者信息

Comolli L R, Pelton J G, Tinoco I

机构信息

Department of Chemistry, University of California at Berkeley and Structural Biology Department, Physical Biosciences Division, Lawrence Berkeley National Laboratory, Berkeley, CA 94720-1460, USA.

出版信息

Nucleic Acids Res. 1998 Oct 15;26(20):4688-95. doi: 10.1093/nar/26.20.4688.

Abstract

An RNA 'kissing' complex is formed by the association of two hairpins via base pairing of their complementary loops. This sense-antisense RNA motif is used in the regulation of many cellular processes, including Escherichia coli ColE1 plasmid copy number. The RNA one modulator protein (Rom) acts as a co-regulator of ColE1 plasmid copy number by binding to the kissing hairpins and stabilizing their interaction. We have used heteronuclear two-dimensional NMR spectroscopy to map the interface between Rom and a kissing complex formed by the loop of the trans -activation response (Tar) element of immunodeficiency virus 1 (HIV-1) and its complement. The protein binding interface was obtained from changes in amide proton signals of uniformly 15N-labeled Rom with increasing concentrations of unlabeled Tar-Tar*. Similarly, the RNA-binding interface was obtained from changes in imino proton signals of uniformly 15N-labeled Tar with increasing concentrations of unlabeled Rom. Our results are in agreement with previous mutagenesis studies and provide additional information on Rom residues involved in RNA binding. The kissing hairpin interface with Rom leads to a model in which the protein contacts the minor groove of the loop-loop helix and, to a lesser extent, the major groove of the stems.

摘要

一种RNA“亲吻”复合物是由两个发夹通过其互补环的碱基配对结合形成的。这种正义-反义RNA基序用于调控许多细胞过程,包括大肠杆菌ColE1质粒的拷贝数。RNA一种调节蛋白(Rom)通过与“亲吻”发夹结合并稳定它们的相互作用,作为ColE1质粒拷贝数的共同调节因子。我们利用异核二维核磁共振光谱绘制了Rom与由免疫缺陷病毒1(HIV-1)反式激活应答(Tar)元件的环及其互补序列形成的“亲吻”复合物之间的界面。蛋白质结合界面是通过随着未标记的Tar-Tar*浓度增加,均匀15N标记的Rom酰胺质子信号的变化获得的。同样,RNA结合界面是通过随着未标记的Rom浓度增加,均匀15N标记的Tar亚氨基质子信号的变化获得的。我们的结果与先前的诱变研究一致,并提供了有关参与RNA结合的Rom残基的额外信息。与Rom的“亲吻”发夹界面产生了一个模型,其中蛋白质与环-环螺旋的小沟接触,并在较小程度上与茎的大沟接触。

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