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Measurements of Single Molecules in Solution and Live Cells Over Longer Observation Times Than Those Currently Possible: The Meaningful Time

机译:溶液和活细胞中单分子的测量时间比目前可能的观察时间长:有意义的时间

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Monitoring translational diffusion of single molecules in solution or in a living cell, particularly DNA and proteins brings valuable information unperturbed by interaction with an artificial surface. The article derives theoretical relationships for time intervals during which just one molecule in the effective probe region can be studied, the time we call meaningful time. This time is greater than the transit time of the molecule through the detection volume, as a single molecule will likely reenter the detection volume several times during measurement. From the infinitely stretched molecular Poisson distribution of single molecules or particles, we select the contribution of the selfsame molecule or particle by applying rules for choosing appropriate statistics for the single-molecule trajectories. The results point to a useful and sensitive predictive power of the derived relationships. The meaningful time relationships are the criteria to check the experimental single molecule data measured under conditions of normal and anomalous Brownian diffusion of the molecules of interest. At femtomolar bulk concentration, it would be possible to observe an individual molecule over a second time interval or longer during which biological processes - and not conformational biophysical changes - are just starting.
机译:监测溶液或活细胞(尤其是DNA和蛋白质)中单个分子的翻译扩散,可以带来与人工表面相互作用而不受干扰的有价值的信息。本文推导了时间间隔的理论关系,在这段时间内可以研究有效探针区域中的一个分子,该时间称为有意义的时间。此时间大于分子通过检测体积的时间,因为单个分子可能会在测量过程中多次重新进入检测体积。从单分子或粒子的无限拉伸的分子泊松分布中,我们通过应用规则为单分子轨迹选择适当的统计量,选择自同分子或粒子的贡献。结果表明派生关系的有用和敏感的预测能力。有意义的时间关系是检查在感兴趣分子的正常和异常布朗扩散条件下测得的实验单分子数据的标准。在飞摩尔堆积浓度下,有可能在第二个时间间隔或更长时间内观察到单个分子,在第二个时间间隔或更长时间内,生物过程才刚刚开始,而不是构象生物物理变化。

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