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Crystallography & NMR system: A new software suite for macromolecular structure determination.晶体学与核磁共振系统:用于大分子结构测定的新软件套件。
Acta Crystallogr D Biol Crystallogr. 1998 Sep 1;54(Pt 5):905-21. doi: 10.1107/s0907444998003254.
2
Binding of the protein kinase PKR to RNAs with secondary structure defects: role of the tandem A-G mismatch and noncontiguous helixes.蛋白激酶PKR与具有二级结构缺陷的RNA的结合:串联A-G错配和非连续螺旋的作用。
Biochemistry. 1998 May 5;37(18):6303-16. doi: 10.1021/bi980113j.
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Refined structure of satellite tobacco mosaic virus at 1.8 A resolution.卫星烟草花叶病毒1.8埃分辨率的精细结构
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A common 40 amino acid motif in eukaryotic RNases H1 and caulimovirus ORF VI proteins binds to duplex RNAs.真核核糖核酸酶H1和花椰菜花叶病毒ORF VI蛋白中常见的40个氨基酸基序可与双链RNA结合。
Nucleic Acids Res. 1998 Apr 1;26(7):1834-40. doi: 10.1093/nar/26.7.1834.
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Crystal structure of the nucleosome core particle at 2.8 A resolution.核小体核心颗粒的晶体结构,分辨率为2.8埃。
Nature. 1997 Sep 18;389(6648):251-60. doi: 10.1038/38444.
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Xlrbpa, a double-stranded RNA-binding protein associated with ribosomes and heterogeneous nuclear RNPs.Xlrbpa,一种与核糖体和不均一核核糖核蛋白相关的双链RNA结合蛋白。
J Cell Biol. 1997 Jul 28;138(2):239-53. doi: 10.1083/jcb.138.2.239.
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Solution structure of (rGGCAGGCC)2 by two-dimensional NMR and the iterative relaxation matrix approach.通过二维核磁共振和迭代弛豫矩阵方法解析(rGGCAGGCC)2的溶液结构
Biochemistry. 1997 Apr 15;36(15):4449-60. doi: 10.1021/bi9625915.
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Comparative mutational analysis of the double-stranded RNA binding domains of Xenopus laevis RNA-binding protein A.非洲爪蟾RNA结合蛋白A双链RNA结合结构域的比较突变分析
J Biol Chem. 1996 Nov 8;271(45):28112-9. doi: 10.1074/jbc.271.45.28112.
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Minor-groove recognition of double-stranded RNA by the double-stranded RNA-binding domain from the RNA-activated protein kinase PKR.RNA激活蛋白激酶PKR的双链RNA结合结构域对双链RNA的小沟识别
Biochemistry. 1996 Aug 6;35(31):9983-94. doi: 10.1021/bi9607259.
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Double-helical RNA in satellite tobacco mosaic virus.烟草花叶病毒卫星中的双螺旋RNA
Nature. 1993 Jan 14;361(6408):179-82. doi: 10.1038/361179a0.

双链RNA与蛋白质相互作用的分子基础:与双链RNA复合的双链RNA结合结构域的结构

Molecular basis of double-stranded RNA-protein interactions: structure of a dsRNA-binding domain complexed with dsRNA.

作者信息

Ryter J M, Schultz S C

机构信息

Department of Chemistry and Biochemistry, University of Colorado, Boulder, CO 80309-0215, USA.

出版信息

EMBO J. 1998 Dec 15;17(24):7505-13. doi: 10.1093/emboj/17.24.7505.

DOI:10.1093/emboj/17.24.7505
PMID:9857205
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1171094/
Abstract

Protein interactions with double-stranded RNA (dsRNA) are critical for many cell processes; however, in contrast to protein-dsDNA interactions, surprisingly little is known about the molecular basis of protein-dsRNA interactions. A large and diverse class of proteins that bind dsRNA do so by utilizing an approximately 70 amino acid motif referred to as the dsRNA-binding domain (dsRBD). We have determined a 1.9 A resolution crystal structure of the second dsRBD of Xenopus laevis RNA-binding protein A complexed with dsRNA. The structure shows that the protein spans 16 bp of dsRNA, interacting with two successive minor grooves and across the intervening major groove on one face of a primarily A-form RNA helix. The nature of these interactions explains dsRBD specificity for dsRNA (over ssRNA or dsDNA) and the apparent lack of sequence specificity. Interestingly, the dsRBD fold resembles a portion of the conserved core structure of a family of polynucleotidyl transferases that includes RuvC, MuA transposase, retroviral integrase and RNase H. Structural comparisons of the dsRBD-dsRNA complex and models proposed for polynucleotidyl transferase-nucleic acid complexes suggest that similarities in nucleic acid binding also exist between these families of proteins.

摘要

蛋白质与双链RNA(dsRNA)的相互作用对许多细胞过程至关重要;然而,与蛋白质 - 双链DNA相互作用相比,令人惊讶的是,人们对蛋白质 - dsRNA相互作用的分子基础知之甚少。一大类与dsRNA结合的蛋白质是通过利用一个约70个氨基酸的基序来实现的,该基序被称为dsRNA结合结构域(dsRBD)。我们已经确定了非洲爪蟾RNA结合蛋白A的第二个dsRBD与dsRNA复合的1.9埃分辨率晶体结构。该结构表明,该蛋白质跨越16个碱基对的dsRNA,与两个连续的小沟相互作用,并横跨主要为A形式RNA螺旋一侧的中间大沟。这些相互作用的性质解释了dsRBD对dsRNA(相对于ssRNA或dsDNA)的特异性以及明显缺乏序列特异性。有趣的是,dsRBD折叠类似于包括RuvC、MuA转座酶、逆转录病毒整合酶和RNase H在内的多核苷酸转移酶家族保守核心结构的一部分。dsRBD - dsRNA复合物与为多核苷酸转移酶 - 核酸复合物提出的模型的结构比较表明,这些蛋白质家族之间在核酸结合方面也存在相似性。