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Calcium-dependent copper redistributions in neuronal cells revealed by a fluorescent copper sensor and X-ray fluorescence microscopy

机译:荧光铜传感器和X射线荧光显微镜显示神经元细胞中钙依赖性铜的重新分布

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摘要

Dynamic fluxes of s-block metals like potassium, sodium, and calcium are of broad importance in cell signaling. In contrast, the concept of mobile transition metals triggered by cell activation remains insufficiently explored, in large part because metals like copper and iron are typically studied as static cellular nutrients and there are a lack of direct, selective methods for monitoring their distributions in living cells. To help meet this need, we now report Coppersensor-3 (CS3), a bright small-molecule fluorescent probe that offers the unique capability to image labile copper pools in living cells at endogenous, basal levels. We use this chemical tool in conjunction with synchotron-based microprobe X-ray fluorescence microscopy (XRFM) to discover that neuronal cells move significant pools of copper from their cell bodies to peripheral processes upon their activation. Moreover, further CS3 and XRFM imaging experiments show that these dynamic copper redistributions are dependent on calcium release, establishing a link between mobile copper and major cell signaling pathways. By providing a small-molecule fluorophore that is selective and sensitive enough to image labile copper pools in living cells under basal conditions, CS3 opens opportunities for discovering and elucidating functions of copper in living systems.
机译:诸如钾,钠和钙等S族金属的动态通量在细胞信号传导中具有重要意义。相比之下,由细胞活化引发的移动过渡金属的概念仍未得到足够的研究,这在很大程度上是因为铜和铁等金属通常作为静态细胞营养物而被研究,并且缺乏直接,选择性的方法来监测其在活细胞中的分布。为了满足这一需求,我们现在报告Coppersensor-3(CS3),这是一种明亮的小分子荧光探针,具有独特的功能,可以对内源性基础水平的活细胞中不稳定的铜池成像。我们将该化学工具与基于同步加速器的微探针X射线荧光显微镜(XRFM)结合使用,以发现神经元细胞在激活后将大量铜从其细胞体移至外围过程。此外,进一步的CS3和XRFM成像实验表明,这些动态的铜重新分布取决于钙的释放,从而在活动铜和主要细胞信号传导途径之间建立了联系。通过提供一种选择性足够灵敏的小分子荧光团,可以在基本条件下成像活细胞中不稳定的铜池,CS3为发现和阐明活系统中铜的功能提供了机会。

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