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Resolution of end-to-end distance distributions of flexible molecules using quenching-induced variations of the Forster distance for fluorescence energy transfer.

机译:使用淬灭诱导的Forster距离的变化引起的柔性分子的端到端距离分布用于荧光能量转移。

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摘要

We describe a new method to recover the distribution of donor-to-acceptor (D-A) distances in flexible molecules using steady-state measurements of the efficiency of fluorescence energy transfer. The method depends upon changes in the Forster distance (Ro) induced by collisional quenching of the donor emission. The Ro-dependent transfer efficiencies are analyzed using nonlinear least squares to recover the mean D-A distance and the width of the distribution. The method was developed and tested using three synthetic D-A pairs, in which the chromophores were separated by alkyl chains of varying lengths. As an example application we also recovered the distribution of distances from the single tryptophan residue in troponin I (trp 158) to acceptor-labeled cysteine 133. The half-width of the distribution increases from 12 A in the native state to 53 A when unfolded by guanidine hydrochloride. For both TnI and the three model compounds the distance distributions recovered from the steady-state transfer efficiencies were in excellent agreement with the distributions recovered using the more sophisticated frequency-domain method (Lakowicz, J.R., M.L. Johnson, W. Wiczk, A. Bhat, and R.F. Steiner. 1987. Chem. Phys. Lett. 138:587-593). The method was found to be reliable and should be generally useful for studies of conformational distributions of macromolecules.
机译:我们描述了一种新的方法来恢复使用荧光能量转移效率的稳态测量在柔性分子中的供体到受体(D-A)距离的分布。该方法取决于施主发射的碰撞猝灭引起的福斯特距离(Ro)的变化。使用非线性最小二乘法分析Ro依赖的传输效率,以恢复平均D-A距离和分布宽度。该方法是使用三对合成D-A对进行开发和测试的,其中生色团由不同长度的烷基链隔开。作为示例应用程序,我们还恢复了从肌钙蛋白I(trp 158)中单个色氨酸残基到受体标记的半胱氨酸133的距离分布。展开时,分布的半宽度从原始状态的12 A增加到53A。由盐酸胍。对于TnI和这三个模型化合物,从稳态转移效率回收的距离分布与使用更复杂的频域方法(Lakowicz,JR,ML Johnson,W。Wiczk,A。Bhat)回收的分布非常吻合。和RF Steiner。1987. Chem。Phys。Lett。138:587-593)。该方法被认为是可靠的,并且通常应用于研究大分子的构象分布。

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