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高分辨率RNA结构

RNA structure at high resolution.

作者信息

Shen L X, Cai Z, Tinoco I

机构信息

Department of Chemistry, University of California, Berkeley 94720, USA.

出版信息

FASEB J. 1995 Aug;9(11):1023-33. doi: 10.1096/fasebj.9.11.7544309.

Abstract

Studies of RNA structural motifs at high resolution by NMR and X-ray crystallographic methods have provided many insights into the fundamental forces that give rise to the unique structural characteristics of RNA. Non-Watson-Crick purine-pyrimidine, purine-purine, and pyrimidine-pyrimidine base pairing, as well as base-phosphate and base-ribose hydrogen bonding, are important forces for folding and stabilizing RNA structures. Base stacking is as important in determining RNA conformations as hydrogen bonding interactions. With the noncanonical interactions, many single-stranded loop regions such as hairpin loops, bulge loops, and internal loops fold into well-defined secondary structures. Loop-loop and loop-helix interactions can produce tertiary structures such as pseudoknots. Also, single strands adjacent to helical regions can form tertiary contacts with base-paired nucleotides of the helices. As we learn more about the structures of the important motifs we can ask more specific questions about the mechanisms of RNA-mediated functions. Conformational flexibility rather than a specific shape of the RNA may be important for some biological reactions. However, knowledge of the structures and the ease of conformational change of the molecules involved in any process are essential for understanding and eventually controlling the process.

摘要

通过核磁共振(NMR)和X射线晶体学方法对RNA结构基序进行的高分辨率研究,为产生RNA独特结构特征的基本作用力提供了许多见解。非沃森-克里克嘌呤-嘧啶、嘌呤-嘌呤和嘧啶-嘧啶碱基配对,以及碱基-磷酸和碱基-核糖氢键,是折叠和稳定RNA结构的重要作用力。碱基堆积在决定RNA构象方面与氢键相互作用同样重要。通过非经典相互作用,许多单链环区域,如发夹环、凸起环和内环,折叠成明确的二级结构。环-环和环-螺旋相互作用可以产生三级结构,如假结。此外,与螺旋区域相邻的单链可以与螺旋中的碱基配对核苷酸形成三级接触。随着我们对重要基序结构的了解越来越多,我们可以就RNA介导功能的机制提出更具体的问题。对于某些生物反应而言,RNA的构象灵活性而非特定形状可能很重要。然而,了解任何过程中涉及的分子结构及其构象变化的难易程度,对于理解并最终控制该过程至关重要。

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