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Quantification and Correction of Systematic Errors Due to Detector Time-Averaging in Single-Molecule Tracking Experiments

机译:在单分子跟踪实验中由于检测器时间平均导致的系统误差的量化和校正

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摘要

Single-molecule tracking is a powerful way to look at the dynamic organization of plasma membranes. However, there are some limitations to its use. For example, it was recently observed, using numerical simulation, that time-averaging effects inherent to the exposure time of detectors are likely to bias the apparent motion of molecules confined in microdomains. Here, we solve this apparently limiting issue analytically. We explore this phenomenon by calculating its effects on the observed diffusion coefficients and domain sizes. We demonstrate that the real parameters can be easily recovered from the measured apparent ones. Interestingly, we find that single-molecule tracking can be used to explore events occurring at a timescale smaller than the exposure time.
机译:单分子跟踪是查看质膜动态组织的有力方法。但是,其使用存在一些限制。例如,最近观察到,使用数值模拟,检测器曝光时间固有的时间平均效应很可能会偏向限制在微区中的分子的表观运动。在这里,我们通过分析解决了这个明显的限制问题。我们通过计算其对观察到的扩散系数和畴尺寸的影响来探索这种现象。我们证明了实际参数可以很容易地从实测值中恢复出来。有趣的是,我们发现单分子跟踪可用于探索以小于暴露时间的时间尺度发生的事件。

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