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互补 RNA 双链体变性的分子机制研究。

Toward a Molecular Mechanism of Complementary RNA Duplexes Denaturation.

机构信息

CNRS Laboratoire de Biochimie Théorique, Institut de Biologie Physico-Chimique, PSL University, Université de Paris, 13 rue Pierre et Marie Curie, 75005, Paris, France.

出版信息

J Phys Chem B. 2023 Jul 13;127(27):6015-6028. doi: 10.1021/acs.jpcb.3c00908. Epub 2023 Jun 30.

Abstract

RNA duplexes are relatively rare but play very important biological roles. As an end-product of template-based RNA replication, they also have key implications for hypothetical primitive forms of life. Unless they are specifically separated by enzymes, these duplexes denature upon a temperature increase. However, mechanistic and kinetic aspects of RNA (and DNA) duplex thermal denaturation remain unclear at the microscopic level. We propose an strategy that probes the thermal denaturation of RNA duplexes and allows for an extensive conformational space exploration along a wide temperature range with atomistic precision. We show that this approach first accounts for the strong sequence and length dependence of the duplexes melting temperature, reproducing the trends seen in the experiments and predicted by nearest-neighbor models. The simulations are then instrumental at providing a molecular picture of the temperature-induced strand separation. The textbook canonical "all-or-nothing" two-state model, very much inspired by the protein folding mechanism, can be nuanced. We demonstrate that a temperature increase leads to significantly distorted but stable structures with extensive base-fraying at the extremities, and that the fully formed duplexes typically do not form around melting. The duplex separation therefore appears as much more gradual than commonly thought.

摘要

RNA 双链结构相对较少,但却发挥着非常重要的生物学作用。作为基于模板的 RNA 复制的终产物,它们对于假设的原始生命形式也具有关键意义。除非被酶专门分离,否则这些双链结构在温度升高时会变性。然而,RNA(和 DNA)双链热变性的机制和动力学方面在微观层面上仍不清楚。我们提出了一种策略,该策略可探测 RNA 双链的热变性,并允许在广泛的温度范围内以原子精度探索广泛的构象空间。我们表明,该方法首先解释了双链体熔化温度的强烈序列和长度依赖性,再现了实验中观察到的趋势以及最近邻模型的预测。然后,模拟在提供温度诱导的链分离的分子图像方面具有重要作用。教科书上经典的“全有或全无”二态模型,非常受蛋白质折叠机制的启发,可以进一步深化。我们证明,温度升高会导致极端处的碱基磨损严重但仍稳定的结构,并且完全形成的双链通常不会在融解时形成。因此,双链体的分离比通常认为的要缓慢得多。

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