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Simple Estimation of Förster Resonance Energy Transfer (FRET) Orientation Factor Distribution in Membranes

机译:膜中福斯特共振能量转移(FRET)取向因子分布的简单估计

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摘要

Because of its acute sensitivity to distance in the nanometer scale, Förster resonance energy transfer (FRET) has found a large variety of applications in many fields of chemistry, physics, and biology. One important issue regarding the correct usage of FRET is its dependence on the donor-acceptor relative orientation, expressed as the orientation factor κ2. Different donor/acceptor conformations can lead to κ2 values in the 0 ≤ κ2 ≤ 4 range. Because the characteristic distance for FRET, R0, is proportional to (κ2)1/6, uncertainties in the orientation factor are reflected in the quality of information that can be retrieved from a FRET experiment. In most cases, the average value of κ2 corresponding to the dynamic isotropic limit (<κ2> = 2/3) is used for computation of R0 and hence donor-acceptor distances and acceptor concentrations. However, this can lead to significant error in unfavorable cases. This issue is more critical in membrane systems, because of their intrinsically anisotropic nature and their reduced fluidity in comparison to most common solvents. Here, a simple numerical simulation method for estimation of the probability density function of κ2 for membrane-embedded donor and acceptor fluorophores in the dynamic regime is presented. In the simplest form, the proposed procedure uses as input the most probable orientations of the donor and acceptor transition dipoles, obtained by experimental (including linear dichroism) or theoretical (such as molecular dynamics simulation) techniques. Optionally, information about the widths of the donor and/or acceptor angular distributions may be incorporated. The methodology is illustrated for special limiting cases and common membrane FRET pairs.
机译:由于其对纳米级距离的敏锐性,福斯特共振能量转移(FRET)已在化学,物理学和生物学的许多领域中找到了广泛的应用。关于正确使用FRET的一个重要问题是其对供体-受体相对取向的依赖性,表达为取向因子κ 2 。不同的供体/受体构象可导致κ 2 的值在0≤κ 2 ≤4的范围内。因为FRET的特征距离R0与(κ 2 1/6 成比例,所以定向因子的不确定性反映在可以检索的信息质量中来自FRET实验。在大多数情况下,对应于动态各向同性极限(<κ 2 > = 2/3)的κ 2 平均值用于计算R0,因此供体-受体距离和受体浓度。但是,这可能会在不利的情况下导致重大错误。由于与大多数普通溶剂相比,其固有的各向异性和流动性降低,因此在膜系统中,此问题更为关键。在此,提出了一种简单的数值模拟方法,用于估计动态嵌入膜的供体和受体荧光团的κ 2 的概率密度函数。以最简单的形式,所提出的程序使用通过实验(包括线性二色性)或理论(例如分子动力学模拟)技术获得的供体和受体跃迁偶极的最可能取向作为输入。可选地,可以结合关于供体和/或受体角度分布的宽度的信息。说明了针对特殊限制情况和常见膜FRET对的方法。

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