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

Sheel C Dodani, Dylan W Domaille, Christine I Nam, Evan W Miller, Lydia A Finney, Stefan Vogt, Christopher J Chang

Department of Chemistry, University of California, Berkeley, CA 94720, USA.

Journal Article: Proceedings of the National Academy of Sciences (impact factor: 9.43). 03/2011; 108(15):5980-5. DOI: 10.1073/pnas.1009932108

Abstract

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.

Source: PubMed

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Keywords

bright small-molecule fluorescent probe
 
broad importance
 
calcium release
 
cell activation
 
cell bodies
 
cell signaling
 
dynamic copper redistributions
 
image labile copper pools
 
insufficiently explored
 
major cell signaling pathways
 
mobile copper
 
mobile transition metals
 
neuronal cells move significant pools
 
peripheral processes
 
s-block metals
 
selective methods
 
small-molecule fluorophore
 
static cellular nutrients
 
unique capability
 
XRFM imaging experiments