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Fe–N–C Artificial Enzyme: Activation of Oxygen for Dehydrogenation and Monoxygenation of Organic Substrates under Mild Condition and Cancer Therapeutic Application

Developing highly efficient biomimetic catalysts that directly use O2 as the terminal oxidant to dehydrogenate and monoxygenate substrates with high selectivity under mild conditions has long been pursued but rarely achieved yet. Herein, we report that heterogeneous Fe–N–C, which is commonly used as...

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Bibliographic Details
Published in:ACS applied materials & interfaces 2018-10, Vol.10 (41), p.35327-35333
Main Authors: He, Fei, Mi, Li, Shen, Yanfei, Mori, Toshiyuki, Liu, Songqin, Zhang, Yuanjian
Format: Article
Language:English
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Summary:Developing highly efficient biomimetic catalysts that directly use O2 as the terminal oxidant to dehydrogenate and monoxygenate substrates with high selectivity under mild conditions has long been pursued but rarely achieved yet. Herein, we report that heterogeneous Fe–N–C, which is commonly used as an electrocatalyst for oxygen reduction reaction, had unusual biomimetic catalytic activity in both dehydrogenation and monoxygenation of a series of organic molecules (∼100% selectivity) by directly using O2. The Fe–N x center was verified to be the active site that reductively activated O2 by spontaneously generating specific reactive oxygen species (ROS) (1O2, O2 •–, and H2O2). Aided by these ROS, under physiological conditions, the Fe–N–C was further successfully exampled to kill proliferative lung cancer cells. Fe–N–C had several striking superior features with respect to natural enzymes, classical heterogeneous nanozymes, and homogeneous artificial enzymes incapable of working under harsh conditions (extreme pH and high temperature), ease of separation and recycling, and direct use of O2. It would open up a new vista of Fe–N–C as an artificial enzyme in biomimetic catalysis, ranging from fundamental simulation of oxidase/oxygenase metabolism to industrial oxidation processes and to disease treatment.
ISSN:1944-8244
1944-8252
DOI:10.1021/acsami.8b15540