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首页> 外文期刊>Chemical science >A novel copper-chelating strategy for fluorescent proteins to image dynamic copper fluctuations on live cell surfaces
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A novel copper-chelating strategy for fluorescent proteins to image dynamic copper fluctuations on live cell surfaces

机译:一种新颖的铜螯合策略,用于荧光蛋白成像活细胞表面上动态铜的波动

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摘要

Copper is indispensable in most aerobic organisms although it is toxic if unregulated as illustrated in many neurodegenerative diseases. To elucidate the mechanisms underlying copper release from cells, a membrane-targeting reporter which can compete with extracellular copper-binding molecules is highly desirable. However, engineering a reporter protein to provide both high sensitivity and selectivity for copper(II) has been challenging, likely due to a lack of proper copper(II)-chelating strategies within proteins. Here, we report a new genetically encoded fluorescent copper(II) reporter by employing a copper-binding tripeptide derived from human serum albumin (HSA), which is one of the major copper-binding proteins in extracellular environments. Optimized insertion of the tripeptide into the green fluorescent protein leads to rapid fluorescence quenching (up to >85% change) upon copper-binding, while other metal ions have no effect. Furthermore, the high binding affinity of the reporter enables reliable copper detection even in the presence of competing biomolecules such as HSA and amyloid beta peptides. We also demonstrate that our reporter proteins can be used to visualize dynamic copper fluctuations on living HeLa cell surfaces.
机译:铜在大多数有氧生物中都是必不可少的,尽管如许多神经退行性疾病所示,如果不加以控制,铜将具有毒性。为了阐明铜从细胞中释放的机理,非常需要能够与细胞外铜结合分子竞争的靶向膜的报道分子。然而,工程化报道蛋白以提供对铜(II)的高灵敏度和选择性一直是具有挑战性的,这可能是由于蛋白质内缺乏适当的铜(II)螯合策略所致。在这里,我们报告了一种新的基因编码的荧光铜(II)报告基因,它采用了源自人血清白蛋白(HSA)的铜结合三肽,这是细胞外环境中的主要铜结合蛋白之一。将三肽最佳地插入绿色荧光蛋白后,在结合铜时会导致快速的荧光淬灭(变化> 85%),而其他金属离子则没有作用。此外,即使在竞争性生物分子(例如HSA和淀粉样β肽)存在的情况下,报道分子的高结合亲和力也能够可靠地检测铜。我们还证明了我们的报告蛋白可用于可视化活HeLa细胞表面上的动态铜波动。

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