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BIMOLECULAR FLUORESCENCE COMPLEMENTATION: VISUALIZATION OF MOLECULAR INTERACTIONS IN LIVING CELLS

机译:双分子荧光互补:活细胞中分子相互作用的可视化

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摘要

A variety of experimental methods have been developed for the analysis of protein interactions. The majority of these methods either require disruption of the cells to detect molecular interactions or rely on indirect detection of the protein interaction. The bimolecular fluorescence complementation (BiFC) assay provides a direct approach for the visualization of molecular interactions in living cells and organisms. The BiFC approach is based on the facilitated association between two fragments of a fluorescent protein when the fragments are brought together by an interaction between proteins fused to the fragments. The BiFC approach has been used for visualization of interactions among a variety of structurally divers interaction partners in many different cell types and. It enables detection of transient complexes as well as complexes formed by a subpopulation of the interaction partners. It is essential to include negative controls in each experiment in which the interface between the interaction partners has been mutated or deleted. The BiFC assay has been adapted for simultaneous visualization of multiple protein complexes in the same cell and the competition for shared interaction partners. A ubiquitin-mediated fluorescence complementation (UbFC) assay has also been developed for visualization of the covalent modification of proteins by ubiquitin family peptides. These fluorescence complementation assays have a great potential to illuminate a variety of biological interactions in the future.
机译:已经开发出多种实验方法来分析蛋白质相互作用。这些方法中的大多数要么需要破坏细胞以检测分子相互作用,要么依赖于蛋白质相互作用的间接检测。双分子荧光互补(BiFC)测定法为可视化活细胞和生物体中的分子相互作用提供了一种直接方法。 BiFC方法基于荧光蛋白的两个片段之间的便利缔合,当两个片段通过融合到片段的蛋白质之间的相互作用而聚集在一起时。 BiFC方法已用于可视化许多不同细胞类型中各种结构多样的相互作用伙伴之间的相互作用。它可以检测瞬态复合物以及由相互作用伙伴亚群形成的复合物。在每个交互伙伴之间的界面已被突变或删除的实验中,必须包括阴性对照。 BiFC分析适用于同时可视化同一细胞中的多种蛋白质复合物以及竞争共享相互作用伙伴。还已经开发了泛素介导的荧光互补(UbFC)测定法,以可视化泛素家族肽对蛋白质的共价修饰。这些荧光互补测定法在将来阐明各种生物相互作用方面具有巨大潜力。

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    Tom K. Kerppola;

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  • 年(卷),期 -1(85),-1
  • 年度 -1
  • 页码 431–470
  • 总页数 37
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