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RNA假结的机械解折叠特性

Characterization of the mechanical unfolding of RNA pseudoknots.

作者信息

Green Lisa, Kim Chul-Hyun, Bustamante Carlos, Tinoco Ignacio

机构信息

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

出版信息

J Mol Biol. 2008 Jan 11;375(2):511-28. doi: 10.1016/j.jmb.2007.05.058. Epub 2007 May 26.

Abstract

The pseudoknot is an important RNA structural element that provides an excellent model system for studying the contributions of tertiary interactions to RNA stability and to folding kinetics. RNA pseudoknots are also of interest because of their key role in the control of ribosomal frameshifting by viral RNAs. Their mechanical properties are directly relevant to their unfolding by ribosomes during translation. We have used optical tweezers to study the kinetics and thermodynamics of mechanical unfolding and refolding of single RNA molecules. Here we describe the unfolding of the frameshifting pseudoknot from infectious bronchitis virus (IBV), three constituent hairpins, and three mutants of the IBV pseudoknot. All four pseudoknots cause -1 programmed ribosomal frameshifting. We have measured the free energies and rates of mechanical unfolding and refolding of the four frameshifting pseudoknots. Our results show that the IBV pseudoknot requires a higher force than its corresponding hairpins to unfold. Furthermore, its rate of unfolding changes little with increasing force, in contrast with the rate of hairpin unfolding. The presence of Mg(2+) significantly increases the kinetic barriers to unfolding the IBV pseudoknot, but has only a minor effect on the hairpin unfolding. The greater mechanical stability of pseudoknots compared to hairpins, and their kinetic insensitivity to force supports the hypothesis that -1 frameshifting depends on the difficulty of unfolding the mRNA.

摘要

假结是一种重要的RNA结构元件,为研究三级相互作用对RNA稳定性和折叠动力学的贡献提供了一个极佳的模型系统。RNA假结还因其在病毒RNA控制核糖体移码中的关键作用而备受关注。它们的力学性质与翻译过程中核糖体使其解折叠直接相关。我们利用光镊研究了单个RNA分子机械解折叠和重新折叠的动力学及热力学。在此,我们描述了传染性支气管炎病毒(IBV)移码假结、三个组成发夹以及IBV假结的三个突变体的解折叠情况。所有这四个假结都会导致-1程序性核糖体移码。我们测量了这四个移码假结的自由能以及机械解折叠和重新折叠的速率。我们的结果表明,IBV假结解折叠所需的力比其相应发夹所需的力更高。此外,与发夹解折叠速率不同,其解折叠速率随力的增加变化不大。Mg(2+)的存在显著增加了IBV假结解折叠的动力学障碍,但对发夹解折叠的影响较小。与发夹相比,假结具有更高的机械稳定性,且其动力学对力不敏感,这支持了-1移码取决于mRNA解折叠难度的假说。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0eb4/7094456/f9065a842775/gr1_lrg.jpg

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