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RNA中氢键网络的能量学:围绕G+1和U42的氢键是发夹状核酶三级结构稳定性的主要决定因素。

Energetics of hydrogen bond networks in RNA: hydrogen bonds surrounding G+1 and U42 are the major determinants for the tertiary structure stability of the hairpin ribozyme.

作者信息

Klostermeier Dagmar, Millar David P

机构信息

Department of Molecular Biology, The Scripps Research Institute, MB-19, 10550 North Torrey Pines Road, La Jolla, California 92037, USA.

出版信息

Biochemistry. 2002 Dec 3;41(48):14095-102. doi: 10.1021/bi025551b.

Abstract

The hairpin ribozyme, a small catalytic RNA consisting of two helix-loop-helix motifs, serves as a paradigm for RNA folding. In the active conformer, the ribozyme is docked into a compact structure via loop-loop interactions. The crystal structure of the docked hairpin ribozyme shows an intricate network of hydrogen bonding interactions at the docking interface, mediated by the base, sugar, and phosphate groups of U42 and G+1 [Rupert, P. B., and Ferre-D'Amare, A. R. (2001) Nature 410, 780-786]. To elucidate the determinants for tertiary structure stability in the hairpin ribozyme, we evaluated the energetic contributions of hydrogen bonds surrounding U42 and G+1 by time-resolved fluorescence resonance energy transfer using modified ribozymes that lack one or more of the individual interactions. Elimination of a single tertiary hydrogen bond consistently resulted in a net destabilization of approximately 2 kJ/mol. The results of double- and triple-mutant cycles suggest that individual hydrogen bonds surrounding G+1 or U42 act cooperatively and form extended hydrogen bond networks that stabilize the docked ribozyme. These results demonstrate that RNAs, similar to proteins, can exploit coupled hydrogen bond networks to stabilize the docking of distant structural domains.

摘要

发夹状核酶是一种由两个螺旋-环-螺旋基序组成的小型催化RNA,是RNA折叠的范例。在活性构象中,核酶通过环-环相互作用对接成紧凑结构。对接后的发夹状核酶的晶体结构显示,在对接界面处存在由U42和G+1的碱基、糖基和磷酸基团介导的复杂氢键相互作用网络[鲁珀特,P.B.,和费雷-达马雷,A.R.(2001年)《自然》410,780-786]。为了阐明发夹状核酶中三级结构稳定性的决定因素,我们使用缺乏一种或多种个体相互作用的修饰核酶,通过时间分辨荧光共振能量转移评估了围绕U42和G+1的氢键的能量贡献。消除单个三级氢键始终导致约2 kJ/mol的净不稳定。双突变和三突变循环的结果表明,围绕G+1或U42的单个氢键协同作用,形成扩展的氢键网络,稳定对接的核酶。这些结果表明,与蛋白质类似,RNA可以利用耦合的氢键网络来稳定远距离结构域的对接。

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