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Macrocyclic Conformational Switch Coupled with Pyridinium-Induced PET for Fluorescence Detection of Adenosine Triphosphate
  • Morozov, Boris S. ;
  • Gargiulo, Fabiano ;
  • Ghule, Swapnil ;
  • Lee, Dong Joon ;
  • Hampel, Frank ;
  • Kim, Hwan Myung ;
  • Kataev, Evgeny A.
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Publication Year
2024-03-13
Publisher
American Chemical Society
Citation
Journal of the American Chemical Society, Vol.146, pp.7105-7115
Mesh Keyword
Adenosine triphosphateAdenosine-5-triphosphateCellular responseConformational switchesDown-streamFluorescence detectionFluorescence enhancementMacrocyclicsPyridiniumSynthetic receptorsAdenosine DiphosphateAdenosine TriphosphateFluorescenceFluorescent DyesHeLa CellsHumansNucleotidesPositron-Emission TomographyProtein ConformationReceptors, ArtificialSpectrometry, Fluorescence
All Science Classification Codes (ASJC)
CatalysisChemistry (all)BiochemistryColloid and Surface Chemistry
Abstract
The binding of nucleotides is crucial for signal transduction as it induces conformational protein changes, leading to downstream cellular responses. Synthetic receptors that bind nucleotides and transduce the binding event into global conformational rearrangements are highly challenging to design, especially those that operate in an aqueous solution. Much work is focused on evaluating functionalized dyes to detect nucleotides, whereas coupling of a nucleotide-induced conformational switching to a sensing event has not been reported to date. We disclose synthetic receptors that undergo a global conformational rearrangement upon nucleotide binding. Integrating naphthalimide and the pyridinium ion into the structure enables stabilization of the folded conformation and efficient fluorescence quenching. The binding of a nucleotide rearranges the receptor conformation and alters the strong fluorescence enhancement. The methylpyridinium-containing receptor demonstrated high sensing selectivity for adenosine 5′-triphosphate (ATP) and a record 160-fold fluorescence enhancement. It can detect fluctuations of ATP in HeLa cells and possesses low cytotoxicity. The developed systems present an attractive approach for designing ATP-responsive artificial molecular switches that operate in water and integrate a strong fluorescence response.
Language
eng
URI
https://dspace.ajou.ac.kr/dev/handle/2018.oak/34003
DOI
https://doi.org/10.1021/jacs.4c01621
Fulltext

Type
Article
Funding
Financial support for this work was provided by DFG grants KA 3444/16-1 and DFG KA3444/25-1. H.M.K. acknowledges grants from the National Research Foundation of Korea (2022R1A2B5B03001607 and 2019R1A5A2026045).
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Kim, Hwan Myung김환명
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