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生物分子折叠的单分子力谱测量中的记忆效应。

Memory effects in single-molecule force spectroscopy measurements of biomolecular folding.

机构信息

Department of Physics, University of Alberta, Edmonton, AB T6G 2E1, Canada.

出版信息

Phys Chem Chem Phys. 2019 Nov 13;21(44):24527-24534. doi: 10.1039/c9cp04197d.

Abstract

Folding is generally assumed to be a Markov process, without memory. When the molecular motion is coupled to that of a probe as in single-molecule force spectroscopy (SMFS) experiments, however, theory predicts that the coupling to a second Markov process should induce memory when monitoring a projection of the full multi-dimensional motion onto a reduced coordinate. We developed a method to evaluate the time constant of the induced memory from its effects on the autocorrelation function, which can be readily determined from experimental data. Applying this method to both simulated SMFS measurements and experimental trajectories of DNA hairpin folding measured by optical tweezers as a model system, we validated the prediction that the linker induces memory. For these measurements, the timescale of the induced memory was found to be similar to the time required for the force probe to respond to changes in the molecule, and in the regime where the experimentally observed dynamics were not significantly perturbed by probe-molecule coupling artifacts. Memory effects are thus a general feature of SMFS measurements induced by the mechanical connection between the molecule and force probe that should be considered when interpreting experimental data.

摘要

折叠通常被认为是一个无记忆的马尔可夫过程。然而,当分子运动与探针的运动耦合时,如在单分子力谱(SMFS)实验中,理论预测当监测全多维运动在约化坐标上的投影时,与第二个马尔可夫过程的耦合应该会产生记忆。我们开发了一种从诱导记忆对自相关函数的影响来评估其时间常数的方法,该方法可以从实验数据中很容易地确定。我们将该方法应用于模拟 SMFS 测量和通过光学镊子测量的 DNA 发夹折叠的实验轨迹,作为模型系统,验证了链接器诱导记忆的预测。对于这些测量,发现诱导记忆的时间尺度与力探针响应分子变化所需的时间相似,并且在实验观察到的动力学没有因探针-分子耦合伪影而显著扰动的范围内。因此,记忆效应是由分子和力探针之间的机械连接引起的 SMFS 测量的一个普遍特征,在解释实验数据时应该考虑到这一点。

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