Multifunctional Gold Nanozyme‐Engineered Amphotericin B for Enhanced Antifungal Infection Therapy

Author:

Jiang Chunmei1,Li Fangping1,Song Pei1,Wen Mengyao2,Yang Saixue1,Tian Geng1,Shao Dongyan1,Shi Junling1,Shang Li2ORCID

Affiliation:

1. Key Laboratory for Space Bioscience and Space Biotechnology School of Life Sciences Northwestern Polytechnical University Xi'an Shaanxi 710072 China

2. State Key Laboratory of Solidification Processing School of Materials Science and Engineering Northwestern Polytechnical University Xi'an Shaanxi 710072 China

Abstract

AbstractChronic wounds of significant severity and acute injuries are highly vulnerable to fungal infections, drastically impeding the expected wound healing trajectory. The clinical use of antifungal therapeutic drug is hampered by poor solubility, high toxicity and adverse reactions, thereby necessitating the urgent development of novel antifungal therapy strategy. Herein, this study proposes a new strategy to enhance the bioactivity of small‐molecule antifungal drugs based on multifunctional metal nanozyme engineering, using amphotericin B (AmB) as an example. AmB‐decorated gold nanoparticles (AmB@AuNPs) are synthesized by a facile one‐pot reaction strategy, and the AmB@AuNPs exhibit superior peroxidase (POD)‐like enzyme activity, with maximal reaction rates (Vmax) 3.4 times higher than that of AuNPs for the catalytic reaction of H2O2. Importantly, the enzyme‐like activity of AuNPs significantly enhanced the antifungal properties of AmB, and the minimum inhibitory concentrations of AmB@AuNPs against Candida albicans (C. albicans) and Saccharomyces cerevisiae (S. cerevisiae) W303 are reduced by 1.6‐fold and 50‐fold, respectively, as compared with AmB alone. Concurrent in vivo studies conducted on fungal‐infected wounds in mice underscored the fundamentally superior antifungal ability and biosafety of AmB@AuNPs. The proposed strategy of engineering antifungal drugs with nanozymes has great potential for enhanced therapy of fungal infections and related diseases.

Funder

National Natural Science Foundation of China

Publisher

Wiley

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