Motion is an essential and fundamental feature of any living organism. The evolved organisms have developed sophisticated and perfect machineries and highly delicate mechanisms to carry out directional and coordinated movements which eventually lead to motion at the macroscopic length scale. By mimicking these natural machineries, attempts to design and synthesize similar molecular motors are made in relevance to their applications in drug delivery, data storage, and molecular sensing. It is highly desirable to establish the rules for controlling the conformational states of molecular motors by tuning some of the external variables which can be used for the design strategies. We contribute to this subject by looking into the solvent influence on the conformational states of a synthetic molecular rotor, namely, diketopyrrolopyrrole (DPP) based [2]rotaxane, using the force-field molecular dynamics approach. We study this system in three different solvents, and we report a strong solvent dependence in the population of three different translational isomers. In chloroform solvent we report the dominant population of the 2-P isomer which is in excellent agreement with experimental results based on H NMR spectra (Org. Lett. 2013, 15, 1274). However, there is a striking difference seen in the population of translational isomers in DMSO solvent, and we attribute these features to negligence of solvent hydrogen bonding induced upfield and downfield effects in the interpretation of experimental proton NMR spectra. In addition, we also report a solvent-polarity-induced fully unstretched to folded conformational transition in the [2]rotaxane system. On the basis of the molecular mechanics Poisson—Boltzmann (and generalized Born) surface area approach, we identify the driving force for the formation of the supramolecuiar guest—host [2]rotaxane system. Finally, we calculate the relative binding free energies for the macrocycle at different binding sites of the DPP skeleton using the molecular dynamics simulations performed for the macrocycle—rotaxane system in water solvent which suggests the increased stability of the 2-0 isomer in polar solvent.
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机译:运动是任何生物体的基本特征。进化出的生物体已经发展出复杂而完善的机械和高度精密的机制,可以进行定向和协调运动,最终导致宏观尺度的运动。通过模仿这些自然机械,尝试设计和合成与它们在药物递送,数据存储和分子传感中的应用相关的类似分子电动机。迫切需要通过调整一些可用于设计策略的外部变量来建立用于控制分子马达的构象状态的规则。通过使用力场分子动力学方法,研究溶剂对合成分子转子即基于二酮吡咯并吡咯(DPP)的[2]轮烷的构象状态的影响,从而为这一问题做出了贡献。我们在三种不同的溶剂中研究了该系统,并且我们在三种不同的翻译异构体中报告了强烈的溶剂依赖性。在氯仿溶剂中,我们报告了2-P异构体的主要种群,这与基于1 H NMR光谱的实验结果非常吻合(Org。Lett。2013,15,1274)。但是,在DMSO溶剂中,翻译异构体的数量存在显着差异,我们将这些特征归因于在解释质子NMR光谱时溶剂氢键引起的上场和下场效应的疏忽。此外,我们还报告了[2]轮烷体系中溶剂极性诱导的完全未拉伸至折叠构象转变。基于泊松-玻尔兹曼(和广义的玻恩)表面积方法的分子力学,我们确定了形成超分子客体-主体[2]轮烷的驱动力。最后,我们使用在水溶剂中对大环-轮烷体系进行的分子动力学模拟,计算了DPP骨架不同结合位点上大环的相对结合自由能,这表明2-0异构体在极性溶剂中的稳定性提高了。
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