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Published September 16, 2020 | Supplemental Material
Journal Article Open

Ligand-Directed Approach to Activity-Based Sensing: Developing Palladacycle Fluorescent Probes That Enable Endogenous Carbon Monoxide Detection

Abstract

Carbon monoxide (CO) is an emerging gasotransmitter and reactive carbon species with broad anti-inflammatory, cytoprotective, and neurotransmitter functions along with therapeutic potential for the treatment of cardiovascular diseases. The study of CO chemistry in biology and medicine relative to other prominent gasotransmitters such as NO and H2S remains challenging, in large part due to limitations in available tools for the direct visualization of this transient and freely diffusing small molecule in complex living systems. Here we report a ligand-directed activity-based sensing (ABS) approach to CO detection through palladium-mediated carbonylation chemistry. Specifically, the design and synthesis of a series of ABS probes with systematic alterations in the palladium-ligand environment (e.g., sp3-S, sp3-N, sp2-N) establish structure–activity relationships for palladacycles to confer selective reactivity with CO under physiological conditions. These fundamental studies led to the development of an optimized probe, termed Carbon Monoxide Probe-3 Ester Pyridine (COP-3E-Py), which enables imaging of CO release in live cell and brain settings, including monitoring of endogenous CO production that triggers presynaptic dopamine release in fly brains. This work provides a unique tool for studying CO in living systems and establishes the utility of a synthetic methods approach to activity-based sensing using principles of organometallic chemistry.

Copyright and License

Copyright © 2020 American Chemical Society

Acknowledgement

We thank the NIH (ES 28096 and ES 4705 to C.J.C.) for funding. J.M. was supported by a fellowship of the German National Academic Foundation (Studienstiftung). D.H. was supported by a fellowship of the Konrad–Adenauer Stiftung. K.J.B. was supported by an NSF graduate fellowship. B.W.M. was supported by an American Heart Association Fellowship. B.W.M. and S.P.R. thank the NSF (CHE-1900482) for funding. We also thank JSPS KAKENHI for funding (17K07122 to K.U., 19H01013 to M.S., and Takeda Science Foundation to K.U.). We thank Ann Fischer (UC Berkeley Tissue Culture Facility) for expert technical assistance. We thank Allegra Aron, Lakshmi Krishnamoorthy, Joseph A. Cotruvo, Jr., Zeming Wang, and Sumin Lee for insightful discussion and experimental assistance.

Additional Information

The Supporting Information is available free of charge at https://pubs.acs.org/doi/10.1021/jacs.0c06405.

  • Experimental details, including characterization of compounds (PDF)

  • Crystallographic data for COP-1 (CIF)

  • Crystallographic data for COP-1-PY (CIF)

  • Crystallographic data for COP-1′ (CIF)

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Additional details

Created:
August 21, 2024
Modified:
August 21, 2024