在反馈跟踪显微镜中进行分子内荧光相关光谱学。
Intramolecular fluorescence correlation spectroscopy in a feedback tracking microscope.
机构信息
Edward L. Ginzton Laboratory, Stanford University, Stanford, California, USA.
出版信息
Biophys J. 2010 Jul 7;99(1):313-22. doi: 10.1016/j.bpj.2010.03.045.
Abstract
We derive the statistics of the signals generated by shape fluctuations of large molecules studied by feedback tracking microscopy. We account for the influence of intramolecular dynamics on the response of the tracking system and derive a general expression for the fluorescence autocorrelation function that applies when those dynamics are linear. We show that in comparison to traditional fluorescence correlation spectroscopy, tracking provides enhanced sensitivity to translational diffusion, molecular size, heterogeneity, and long-timescale decays. We demonstrate our approach using a three-dimensional tracking microscope to study genomic lambda-phage DNA molecules with various fluorescence label configurations.
摘要
我们推导出了通过反馈跟踪显微镜研究的大分子形状波动产生的信号的统计特性。我们考虑了分子内动力学对跟踪系统响应的影响,并推导出了适用于这些动力学为线性时的荧光自相关函数的一般表达式。我们表明,与传统的荧光相关光谱学相比,跟踪提供了对平动扩散、分子大小、异质性和长时间尺度衰减的更高灵敏度。我们使用三维跟踪显微镜研究了具有不同荧光标记配置的基因组 lambda 噬菌体 DNA 分子,展示了我们的方法。
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