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Spatial engineering of single-atom Fe adjacent to Cu-assisted nanozymes for biomimetic O2 activation.


ABSTRACT: The precise design of single-atom nanozymes (SAzymes) and understanding of their biocatalytic mechanisms hold great promise for developing ideal bio-enzyme substitutes. While considerable efforts have been directed towards mimicking partial bio-inspired structures, the integration of heterogeneous SAzymes configurations and homogeneous enzyme-like mechanism remains an enormous challenge. Here, we show a spatial engineering strategy to fabricate dual-sites SAzymes with atomic Fe active center and adjacent Cu sites. Compared to planar Fe-Cu dual-atomic sites, vertically stacked Fe-Cu geometry in FePc@2D-Cu-N-C possesses highly optimized scaffolds, favorable substrate affinity, and fast electron transfer. These characteristics of FePc@2D-Cu-N-C SAzyme induces biomimetic O2 activation through homogenous enzymatic pathway, resembling functional and mechanistic similarity to natural cytochrome c oxidase. Furthermore, it presents an appealing alternative of cytochrome P450 3A4 for drug metabolism and drug-drug interaction. These findings are expected to deepen the fundamental understanding of atomic-level design in next-generation bio-inspired nanozymes.

SUBMITTER: Wang Y 

PROVIDER: S-EPMC10933453 | biostudies-literature | 2024 Mar

REPOSITORIES: biostudies-literature

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Spatial engineering of single-atom Fe adjacent to Cu-assisted nanozymes for biomimetic O<sub>2</sub> activation.

Wang Ying Y   Paidi Vinod K VK   Wang Weizhen W   Wang Yong Y   Jia Guangri G   Yan Tingyu T   Cui Xiaoqiang X   Cai Songhua S   Zhao Jingxiang J   Lee Kug-Seung KS   Lee Lawrence Yoon Suk LYS   Wong Kwok-Yin KY  

Nature communications 20240312 1


The precise design of single-atom nanozymes (SAzymes) and understanding of their biocatalytic mechanisms hold great promise for developing ideal bio-enzyme substitutes. While considerable efforts have been directed towards mimicking partial bio-inspired structures, the integration of heterogeneous SAzymes configurations and homogeneous enzyme-like mechanism remains an enormous challenge. Here, we show a spatial engineering strategy to fabricate dual-sites SAzymes with atomic Fe active center and  ...[more]

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