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Understanding the mechanical response of double- stranded DNA and RNA under constant stretching forces using all-atom molecular dynamics

机译:使用全原子分子动力学了解在恒定拉伸力下双链DNA和RNA的机械响应

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摘要

Multiple biological processes involve the stretching of nucleic acids (NAs). Stretching forces induce local changes in the molecule structure, inhibiting or promoting the binding of proteins, which ultimately affects their functionality. Understanding how a force induces changes in the structure of NAs at the atomic level is a challenge. Here, we use all-atom, microsecond-long molecular dynamics to simulate the structure of dsDNA and dsRNA subjected to stretching forces up to 20 pN. We determine all of the elastic constants of dsDNA and dsRNA and provide an explanation for three striking differences in the mechanical response of these two molecules: the threefold softer stretching constant obtained for dsRNA, the opposite twist-stretch coupling, and its nontrivial force dependence. The lower dsRNA stretching resistance is linked to its more open structure, whereas the opposite twist-stretch coupling of both molecules is due to the very different evolution of molecules' interstrand distance with the stretching force. A reduction of this distance leads to overwinding in dsDNA. In contrast, dsRNA is not able to reduce its interstrand distance and can only elongate by unwinding. Interstrand distance is directly correlated with the slide base-pair parameter and its different behavior in dsDNA and dsRNA traced down to changes in the sugar pucker angle of these NAs.
机译:多种生物学过程涉及核酸(NA)的拉伸。拉伸力会引起分子结构的局部变化,从而抑制或促进蛋白质的结合,最终影响其功能。理解力如何在原子水平上诱导NAs结构的变化是一个挑战。在这里,我们使用全原子,微秒长的分子动力学来模拟dsDNA和dsRNA的结构,该结构承受高达20 pN的拉伸力。我们确定了dsDNA和dsRNA的所有弹性常数,并为这两个分子的机械反应中的三个显着差异提供了解释:为dsRNA获得的三倍柔软拉伸常数,相反的扭转-拉伸偶联及其非平凡的力依赖性。较低的dsRNA拉伸抗性与其更开放的结构有关,而两个分子相反的扭曲-拉伸偶联是由于分子的链间距离随拉伸力的变化非常不同。该距离的减小导致dsDNA的过度缠绕。相反,dsRNA不能减少其链间距离,只能通过展开来延长。链间距离与滑动碱基对参数直接相关,其在dsDNA和dsRNA中的不同行为可追溯到这些NA的糖折叠角的变化。

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