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拥挤环境中纳米结构导致的多种扩散机制。

Multiple diffusion mechanisms due to nanostructuring in crowded environments.

作者信息

Sanabria Hugo, Kubota Yoshihisa, Waxham M Neal

机构信息

Department of Neurobiology and Anatomy, University of Texas Health Science Center at Houston, Houston, Texas 77030, USA.

出版信息

Biophys J. 2007 Jan 1;92(1):313-22. doi: 10.1529/biophysj.106.090498. Epub 2006 Oct 13.

Abstract

One of the key questions regarding intracellular diffusion is how the environment affects molecular mobility. Mostly, intracellular diffusion has been described as hindered, and the physical reasons for this behavior are: immobile barriers, molecular crowding, and binding interactions with immobile or mobile molecules. Using results from multi-photon fluorescence correlation spectroscopy, we describe how immobile barriers and crowding agents affect translational mobility. To study the hindrance produced by immobile barriers, we used sol-gels (silica nanostructures) that consist of a continuous solid phase and aqueous phase in which fluorescently tagged molecules diffuse. In the case of molecular crowding, translational mobility was assessed in increasing concentrations of 500 kDa dextran solutions. Diffusion of fluorescent tracers in both sol-gels and dextran solutions shows clear evidence of anomalous subdiffusion. In addition, data from the autocorrelation function were analyzed using the maximum entropy method as adapted to fluorescence correlation spectroscopy data and compared with the standard model that incorporates anomalous diffusion. The maximum entropy method revealed evidence of different diffusion mechanisms that had not been revealed using the anomalous diffusion model. These mechanisms likely correspond to nanostructuring in crowded environments and to the relative dimensions of the crowding agent with respect to the tracer molecule. Analysis with the maximum entropy method also revealed information about the degree of heterogeneity in the environment as reported by the behavior of diffusive molecules.

摘要

关于细胞内扩散的关键问题之一是环境如何影响分子移动性。大多数情况下,细胞内扩散被描述为受阻,这种行为的物理原因包括:固定障碍物、分子拥挤以及与固定或移动分子的结合相互作用。利用多光子荧光相关光谱的结果,我们描述了固定障碍物和拥挤剂如何影响平移移动性。为了研究固定障碍物产生的阻碍,我们使用了溶胶 - 凝胶(二氧化硅纳米结构),它由连续的固相和水相组成,荧光标记的分子在其中扩散。在分子拥挤的情况下,在浓度不断增加的500 kDa葡聚糖溶液中评估平移移动性。荧光示踪剂在溶胶 - 凝胶和葡聚糖溶液中的扩散都显示出明显的反常亚扩散证据。此外,使用适用于荧光相关光谱数据的最大熵方法分析自相关函数的数据,并与包含反常扩散的标准模型进行比较。最大熵方法揭示了使用反常扩散模型未发现的不同扩散机制的证据。这些机制可能对应于拥挤环境中的纳米结构以及拥挤剂相对于示踪分子的相对尺寸。用最大熵方法进行的分析还揭示了关于环境异质性程度的信息,这是由扩散分子的行为报告的。

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本文引用的文献

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Anomalous diffusion of proteins due to molecular crowding.由于分子拥挤导致的蛋白质异常扩散。
Biophys J. 2005 Nov;89(5):2960-71. doi: 10.1529/biophysj.104.051078. Epub 2005 Aug 19.
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