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Expanding the utility of β-galactosidase complementation: Piece by piece

机译:扩展β-半乳糖苷酶互补作用:逐段

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摘要

The ability to image and quantify multiple biomarkers in disease necessitates the development of split reporter fragment platforms. We have divided the β-galactosidase enzyme into unique, independent polypeptides that are able to reassemble and complement enzymatic activity in bacteria and in mammalian cells. We created two sets of complementing pairs that individually have no enzymatic activity. However, when brought into close geometric proximity, the complementing pairs associated resulting in detectable enzymatic activity. We then constructed a stable ligand complex composed of reporter fragment, linker, and targeting moiety. The targeting moiety, in this case a ligand, allowed cell surface receptor targeting in vitro. Further, we were able to simultaneously visualize two cell surface receptors implicated in cancer development, epidermal growth factor receptor and transferrin receptor, using complementing pairs of the ligand-reporter fragment complex.
机译:对疾病中的多种生物标志物进行成像和定量的能力需要开发分裂的报告片段平台。我们已经将β-半乳糖苷酶分为独特的,独立的多肽,它们能够在细菌和哺乳动物细胞中重组和补充酶促活性。我们创建了两组互补的对,它们分别没有酶活性。然而,当紧密接近几何关系时,相关的互补对导致可检测的酶活性。然后,我们构建了一个稳定的配体复合物,该复合物由报告片段,接头和靶向部分组成。靶向部分,在这种情况下是配体,允许细胞表面受体在体外靶向。此外,我们能够使用配体-报告片段复合物的互补对,同时可视化涉及癌症发展的两个细胞表面受体,表皮生长因子受体和转铁蛋白受体。

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