Aptamer-Modified Cu2+-Functionalized C‑Dots: Versatile Means to Improve Nanozyme Activities-“Aptananozymes”

Aptamer-Modified Cu2+-Functionalized C‑Dots: Versatile Means to Improve Nanozyme Activities-“Aptananozymes”

The covalent linkage of aptamer binding sites to nanoparticle nanozymes is introduced as a versatile method to improve the catalytic activity of nanozymes by concentrating the reaction substrates at the catalytic nanozyme core, thereby emulating the binding and catalytic active-site functions of nat...

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Bibliographic Details
Published in:Journal of the American Chemical Society Vol. 143; no. 30; pp. 11510 - 11519
Main Authors: Ouyang, Yu, Biniuri, Yonatan, Fadeev, Michael, Zhang, Pu, Carmieli, Raanan, Vázquez-González, Margarita, Willner, Itamar
Format: Journal Article
Language:English
Published: American Chemical Society 04-08-2021
Online Access:Get full text
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Summary:The covalent linkage of aptamer binding sites to nanoparticle nanozymes is introduced as a versatile method to improve the catalytic activity of nanozymes by concentrating the reaction substrates at the catalytic nanozyme core, thereby emulating the binding and catalytic active-site functions of native enzymes. The concept is exemplified with the synthesis of Cu2+ ion-functionalized carbon dots (C-dots), modified with the dopamine binding aptamer (DBA) or the tyrosinamide binding aptamer (TBA), for the catalyzed oxidation of dopamine to aminochrome by H2O2 or the oxygenation of l-tyrosinamide to the catechol product, which is subsequently oxidized to amidodopachrome, in the presence of H2O2/ascorbate mixture. Sets of structurally functionalized DBA-modified Cu2+ ion-functionalized C-dots or sets of structurally functionalized TBA-modified Cu2+ ion-functionalized C-dots are introduced as nanozymes of superior catalytic activities (aptananozymes) toward the oxidation of dopamine or the oxygenation of l-tyrosinamide, respectively. The aptananozymes reveal enhanced catalytic activities as compared to the separated catalyst and respective aptamer constituents. The catalytic functions of the aptananozymes are controlled by the structure of the aptamer units linked to the Cu2+ ion-functionalized C-dots. In addition, the aptananozyme shows chiroselective catalytic functions demonstrated by the chiroselective-catalyzed oxidation of l/d-DOPA to l/d-dopachrome. Binding studies of the substrates to the different aptananozymes and mechanistic studies associated with the catalytic transformations are discussed.
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ISSN:0002-7863
1520-5126
DOI:10.1021/jacs.1c03939