OregonFluor enables quantitative intracellular paired agent imaging to assess drug target availability in live cells and tissues

Lei G. Wang; Antonio R. Montaño; Jason R. Combs; Nathan P. McMahon; Allison Solanki; Michelle M. Gomes; Kai Tao; William H. Bisson; Dani A. Szafran; Kimberley S. Samkoe; Kenneth M. Tichauer; Summer L. Gibbs

doi:10.1038/s41557-023-01173-6

OregonFluor enables quantitative intracellular paired agent imaging to assess drug target availability in live cells and tissues

Lei G. Wang, Antonio R. Montaño, Jason R. Combs, Nathan P. McMahon, Allison Solanki, Michelle M. Gomes, Kai Tao, William H. Bisson, Dani A. Szafran, Kimberley S. Samkoe, Kenneth M. Tichauer, Summer L. Gibbs

Research output: Contribution to journal › Article › peer-review

10 Scopus citations

Abstract

Non-destructive fluorophore diffusion across cell membranes to provide an unbiased fluorescence intensity readout is critical for quantitative imaging applications in live cells and tissues. Commercially available small-molecule fluorophores have been engineered for biological compatibility, imparting high water solubility by modifying rhodamine and cyanine dye scaffolds with multiple sulfonate groups. The resulting net negative charge, however, often renders these fluorophores cell-membrane-impermeant. Here we report the design and development of our biologically compatible, water-soluble and cell-membrane-permeable fluorophores, termed OregonFluor (ORFluor). By adapting previously established ratiometric imaging methodology using bio-affinity agents, it is now possible to use small-molecule ORFluor-labelled therapeutic inhibitors to quantitatively visualize their intracellular distribution and protein target-specific binding, providing a chemical toolkit for quantifying drug target availability in live cells and tissues. [Figure not available: see fulltext.].

Original language	English (US)
Pages (from-to)	729-739
Number of pages	11
Journal	Nature Chemistry
Volume	15
Issue number	5
DOIs	https://doi.org/10.1038/s41557-023-01173-6
State	Published - May 2023

ASJC Scopus subject areas

General Chemistry
General Chemical Engineering

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Wang, L. G., Montaño, A. R., Combs, J. R., McMahon, N. P., Solanki, A., Gomes, M. M., Tao, K., Bisson, W. H., Szafran, D. A., Samkoe, K. S., Tichauer, K. M., & Gibbs, S. L. (2023). OregonFluor enables quantitative intracellular paired agent imaging to assess drug target availability in live cells and tissues. Nature Chemistry, 15(5), 729-739. https://doi.org/10.1038/s41557-023-01173-6

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abstract = "Non-destructive fluorophore diffusion across cell membranes to provide an unbiased fluorescence intensity readout is critical for quantitative imaging applications in live cells and tissues. Commercially available small-molecule fluorophores have been engineered for biological compatibility, imparting high water solubility by modifying rhodamine and cyanine dye scaffolds with multiple sulfonate groups. The resulting net negative charge, however, often renders these fluorophores cell-membrane-impermeant. Here we report the design and development of our biologically compatible, water-soluble and cell-membrane-permeable fluorophores, termed OregonFluor (ORFluor). By adapting previously established ratiometric imaging methodology using bio-affinity agents, it is now possible to use small-molecule ORFluor-labelled therapeutic inhibitors to quantitatively visualize their intracellular distribution and protein target-specific binding, providing a chemical toolkit for quantifying drug target availability in live cells and tissues. [Figure not available: see fulltext.].",

author = "Wang, {Lei G.} and Monta{\~n}o, {Antonio R.} and Combs, {Jason R.} and McMahon, {Nathan P.} and Allison Solanki and Gomes, {Michelle M.} and Kai Tao and Bisson, {William H.} and Szafran, {Dani A.} and Samkoe, {Kimberley S.} and Tichauer, {Kenneth M.} and Gibbs, {Summer L.}",

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AU - McMahon, Nathan P.

AU - Solanki, Allison

AU - Gomes, Michelle M.

AU - Tao, Kai

AU - Bisson, William H.

AU - Szafran, Dani A.

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AU - Tichauer, Kenneth M.

AU - Gibbs, Summer L.

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AB - Non-destructive fluorophore diffusion across cell membranes to provide an unbiased fluorescence intensity readout is critical for quantitative imaging applications in live cells and tissues. Commercially available small-molecule fluorophores have been engineered for biological compatibility, imparting high water solubility by modifying rhodamine and cyanine dye scaffolds with multiple sulfonate groups. The resulting net negative charge, however, often renders these fluorophores cell-membrane-impermeant. Here we report the design and development of our biologically compatible, water-soluble and cell-membrane-permeable fluorophores, termed OregonFluor (ORFluor). By adapting previously established ratiometric imaging methodology using bio-affinity agents, it is now possible to use small-molecule ORFluor-labelled therapeutic inhibitors to quantitatively visualize their intracellular distribution and protein target-specific binding, providing a chemical toolkit for quantifying drug target availability in live cells and tissues. [Figure not available: see fulltext.].

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OregonFluor enables quantitative intracellular paired agent imaging to assess drug target availability in live cells and tissues

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