Nanostructured Interface Loaded with Chimeric Enzymes for Fluorimetric Quantification of Cyclosporine A and FK506

Wells, Paulina K., Smutok, Oleh, , , & Katz, Evgeny (2022) Nanostructured Interface Loaded with Chimeric Enzymes for Fluorimetric Quantification of Cyclosporine A and FK506. Analytical Chemistry, 94(20), pp. 7303-7310.

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Description

Advances in protein engineering resulted in increased efforts to create protein biosensors that can replace instrumentation-heavy analytical and diagnostic methods. Sensitivity, amenability to multiplexing, and manufacturability remain to be among the key issues preventing broad utilization of protein biosensors. Here, we attempt to address these by constructing arrays utilizing protein biosensors based on the artificial allosteric variant of PQQ-glucose dehydrogenase (GDH). We demonstrated that the silica nanoparticle-immobilized GDH protein could be deposited on fiberglass sheets without loss of activity. The particle-associated GDH activity could be monitored using changes in the fluorescence of the commonly used electron mediator phenazine methosulfate. The constructed biosensor arrays of macrocyclic immunosuppressant drugs cyclosporine A and FK-506 displayed very low background and a remarkable dynamic range exceeding 300-fold that resulted in a limit of detection of 2 pM for both analytes. This enabled us to quantify both drugs in human blood, serum, urine, and saliva. The arrays could be stored in dry form and quantitatively imaged using a smartphone camera, demonstrating the method's suitability for field and point-of-care applications. The developed approach provides a generalizable platform for biosensor array development that is compatible with inexpensive and potentially scalable manufacturing.

Impact and interest:

4 citations in Scopus
2 citations in Web of Science®
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ID Code: 240327
Item Type: Contribution to Journal (Journal Article)
Refereed: Yes
ORCID iD:
Guo, Zhongorcid.org/0000-0003-0285-5021
Alexandrov, Kirillorcid.org/0000-0002-0957-6511
Additional Information: Funding Information: This work was supported by the Human Frontiers Science Program (HFSP) project grant RGP0002/2018 to O.S., K.A., and E.K. This work was also supported in part by the Australian Research Council Discovery Project DP150100936, as well as NHMRC grant APP1113262 to K.A. K.A. gratefully acknowledges the financial support of QUT/CSIRO Synthetic Biology alliance.
Measurements or Duration: 8 pages
DOI: 10.1021/acs.analchem.2c00650
ISSN: 0003-2700
Pure ID: 135681235
Divisions: Current > Research Centres > Centre for Agriculture and the Bioeconomy
Current > QUT Faculties and Divisions > Faculty of Science
Current > Schools > School of Biology & Environmental Science
Funding Information: This work was supported by the Human Frontiers Science Program (HFSP) project grant RGP0002/2018 to O.S., K.A., and E.K. This work was also supported in part by the Australian Research Council Discovery Project DP150100936, as well as NHMRC grant APP1113262 to K.A. K.A. gratefully acknowledges the financial support of QUT/CSIRO Synthetic Biology alliance.
Copyright Owner: 2022 American Chemical Society
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Deposited On: 08 Jun 2023 03:55
Last Modified: 12 May 2024 21:28