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Förster Resonance Energy Transfer (FRET) between Heterogeneously Distributed Probes: Application to Lipid Nanodomains and Pores

机译:异构探针之间的Förster共振能量转移(FRET):在脂质纳米域和孔中的应用

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摘要

The formation of membrane heterogeneities, e.g., lipid domains and pores, leads to a redistribution of donor (D) and acceptor (A) molecules according to their affinity to the structures formed and the remaining bilayer. If such changes sufficiently influence the Förster resonance energy transfer (FRET) efficiency, these changes can be further analyzed in terms of nanodomain/pore size. This paper is a continuation of previous work on this theme. In particular, it is demonstrated how FRET experiments should be planned and how data should be analyzed in order to achieve the best possible resolution. The limiting resolution of domains and pores are discussed simultaneously, in order to enable direct comparison. It appears that choice of suitable donor/acceptor pairs is the most crucial step in the design of experiments. For instance, it is recommended to use DA pairs, which exhibit an increased affinity to pores (i.e., partition coefficients KD,A > 10) for the determination of pore sizes with radii comparable to the Förster radius R0. On the other hand, donors and acceptors exhibiting a high affinity to different phases are better suited for the determination of domain sizes. The experimental setup where donors and acceptors are excluded from the domains/pores should be avoided.
机译:膜异质性(例如脂质结构域和孔)的形成导致供体(D)和受体(A)分子根据它们对形成的结构和剩余双层的亲和力而重新分布。如果这样的变化足以影响Förster共振能量转移(FRET)效率,则可以根据纳米域/孔的大小进一步分析这些变化。本文是该主题先前工作的延续。特别是,它演示了如何计划FRET实验以及应该如何分析数据以获得最佳分辨率。为了能够进行直接比较,同时讨论了区域和孔的极限分辨率。似乎选择合适的供体/受体对是实验设计中最关键的步骤。例如,建议使用DA对,它们对孔的亲和力增加(即分配系数KD,A> 10),以确定具有与Förster半径R0相当的半径的孔径。另一方面,对不同相表现出高亲和力的供体和受体更适合于确定域大小。应避免将供体和受体从域/孔中排除的实验装置。

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