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Combining chemical and genetic approaches for development of responsive FRET-based sensor systems for protein kinases

机译:结合化学和遗传方法来开发基于反应性FRET的蛋白激酶传感器系统

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Chemical and genetic approaches were combined for the development of responsive FRET-based sensor systems for protein kinases, using PIM2 as the model kinase. Fusions of PIM2 and a red fluorescent protein, TagRFP were expressed in mammalian cells and small-molecule ARC-Lum photoluminescent probes possessing different phosphorescent and fluorescent properties were constructed. Based on a variety of Forster-type resonant energy transfer (FRET) mechanisms (including intermolecular or intramolecular energy transfer and transfer between singlet-singlet or triplet-singlet electronic states of interacting luminophores) of the probe and that of the fluorescently tagged PIM2, FRET-based sensor systems were constructed. The developed assays can be applied for analysis of PIM2 in biological samples and screening and characterization of PIM2 inhibitors in cell lysates. In screening studies sub-micromolar affinity of a D-arginine-rich peptide, nona(D-arginine) amide [(D-Arg)(9)-NH2], towards PIM2 was discovered that points to possible specific effect of this widely used transport peptide to cellular protein phosphorylation balance. (C) 2016 Elsevier B.V. All rights reserved.
机译:化学和遗传方法相结合,使用PIM2作为模型激酶,开发了基于响应式FRET的蛋白激酶传感器系统。在哺乳动物细胞中表达了PIM2和红色荧光蛋白TagRFP的融合体,并构建了具有不同磷光和荧光特性的小分子ARC-Lum光致发光探针。基于探针和荧光标记的PIM2,FRET的多种Forster型共振能量转移(FRET)机制(包括分子间或分子内能量转移以及相互作用的发光体的单重态或三重态-单重态之间的转移)构造了基于传感器的传感器系统。所开发的测定方法可用于分析生物样品中的PIM2以及细胞裂解物中PIM2抑制剂的筛选和表征。在筛选研究中,发现富含D-精氨酸的肽,壬基(D-精氨酸)酰胺[(D-Arg)(9)-NH2]对PIM2的亚微摩尔亲和力表明了这种广泛使用的可能的特定作用转运肽至细胞蛋白磷酸化平衡。 (C)2016 Elsevier B.V.保留所有权利。

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