Activity-Based Sensing with a Metal-Directed Acyl Imidazole Strategy Reveals Cell Type-Dependent Pools of Labile Brain Copper

化学 神经退行性变 小胶质细胞 铜缺乏 电池类型 铜毒性 细胞 生物物理学 细胞内 细胞生物学 生物化学 神经科学 炎症 生物 有机化学 病理 免疫学 医学 疾病
作者
Sumin Lee,Clive Yik‐Sham Chung,Lei Pei,Laura Crăciun,Yuki Nishikawa,Kevin J. Bruemmer,Itaru Hamachi,Kaoru Saijo,Evan W. Miller,Christopher J. Chang
出处
期刊:Journal of the American Chemical Society [American Chemical Society]
卷期号:142 (35): 14993-15003 被引量:45
标识
DOI:10.1021/jacs.0c05727
摘要

Copper is a required nutrient for life and particularly important to the brain and central nervous system. Indeed, copper redox activity is essential to maintaining normal physiological responses spanning neural signaling to metabolism, but at the same time copper misregulation is associated with inflammation and neurodegeneration. As such, chemical probes that can track dynamic changes in copper with spatial resolution, especially in loosely bound, labile forms, are valuable tools to identify and characterize its contributions to healthy and disease states. In this report, we present an activity-based sensing (ABS) strategy for copper detection in live cells that preserves spatial information by a copper-dependent bioconjugation reaction. Specifically, we designed copper-directed acyl imidazole dyes that operate through copper-mediated activation of acyl imidazole electrophiles for subsequent labeling of proximal proteins at sites of elevated labile copper to provide a permanent stain that resists washing and fixation. To showcase the utility of this new ABS platform, we sought to characterize labile copper pools in the three main cell types in the brain: neurons, astrocytes, and microglia. Exposure of each of these cell types to physiologically relevant stimuli shows distinct changes in labile copper pools. Neurons display translocation of labile copper from somatic cell bodies to peripheral processes upon activation, whereas astrocytes and microglia exhibit global decreases and increases in intracellular labile copper pools, respectively, after exposure to inflammatory stimuli. This work provides foundational information on cell type-dependent homeostasis of copper, an essential metal in the brain, as well as a starting point for the design of new activity-based probes for metals and other dynamic signaling and stress analytes in biology.
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