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生物素结合假结的1.3埃晶体结构及RNA分子识别的基础。

The 1.3 A crystal structure of a biotin-binding pseudoknot and the basis for RNA molecular recognition.

作者信息

Nix J, Sussman D, Wilson C

机构信息

Department of Biology and Center for the Molecular Biology of RNA, Sinsheimer Laboratories, University of California at Santa Cruz, Santa Cruz, CA 95064, USA.

出版信息

J Mol Biol. 2000 Mar 10;296(5):1235-44. doi: 10.1006/jmbi.2000.3539.

DOI:10.1006/jmbi.2000.3539
PMID:10698630
Abstract

A pseudoknot-containing aptamer isolated from a pool of random sequence molecules has been shown previously to represent an optimal RNA solution to the problem of binding biotin. The affinity of this RNA molecule is nonetheless orders of magnitude weaker than that of its highly evolved protein analogs, avidin and streptavidin. To understand the structural basis for biotin binding and to compare directly strategies for ligand recognition available to proteins and RNA molecules, we have determined the 1.3 A crystal structure of the aptamer complexed with its ligand. Biotin is bound at the interface between the pseudoknot's stacked helices in a pocket defined almost entirely by base-paired nucleotides. In comparison to the protein avidin, the aptamer packs more tightly around the biotin headgroup and makes fewer contacts with its fatty acid tail. Whereas biotin is deeply buried within the hydrophobic core in the avidin complex, the aptamer relies on a combination of hydrated magnesium ions and immobilized water molecules to surround its ligand. In addition to demonstrating fundamentally different approaches to molecular recognition by proteins and RNA, the structure provides general insight into the mechanisms by which RNA function is mediated by divalent metals.

摘要

先前已证明,从随机序列分子库中分离出的一种含假结的适体是结合生物素问题的最佳RNA解决方案。然而,这种RNA分子的亲和力比其高度进化的蛋白质类似物抗生物素蛋白和链霉抗生物素蛋白弱几个数量级。为了了解生物素结合的结构基础,并直接比较蛋白质和RNA分子用于配体识别的策略,我们确定了与配体复合的适体的1.3埃晶体结构。生物素结合在假结堆叠螺旋之间的界面处,位于一个几乎完全由碱基配对核苷酸定义的口袋中。与蛋白质抗生物素蛋白相比,适体围绕生物素头部基团的堆积更紧密,与脂肪酸尾部的接触更少。在抗生物素蛋白复合物中,生物素深埋在疏水核心内,而适体则依靠水合镁离子和固定水分子的组合来包围其配体。该结构除了展示了蛋白质和RNA在分子识别上的根本不同方法外,还为二价金属介导RNA功能的机制提供了总体见解。

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