Light‐Activated Nanocatalyst for Precise In‐Situ Antimicrobial Synthesis via Photoredox‐Catalytic Click Reaction

Author:

Zhao Minyang1,Cao Lei23,Bai Qingqing1,Lu Yaru4,Li Bowen5,Wu Wenbo4,Ye Jinzhou6,Chen Xinhan6,Wang Zhihong5,Liu Bin23ORCID,Mao Duo1

Affiliation:

1. Department of Laboratory Medicine, Institute of Precision Medicine The First Affiliated Hospital of Sun Yat-Sen University Sun Yat-Sen University 1510080 Guangzhou China

2. Department of Chemical and Biomolecular Engineering National University of Singapore 117585 Singapore Singapore

3. Joint School of National University of Singapore and Tianjin University International Campus of Tianjin University 350207 Fuzhou China

4. Department of Chemistry, Institute of Molecular Aggregation Science Tianjin University 300072 Tianjin China

5. Institute of Transplant Medicine School of Medicine Nankai University 300071 Tianjin China

6. Institute of Infectious Diseases Shenzhen Bay Laboratory 518132 Shenzhen, Guangdong China

Abstract

AbstractThe excessive and prolonged use of antibiotics contributes to the emergence of drug‐resistant S. aureus strains and potential dysbacteriosis‐related diseases, necessitating the exploration of alternative therapeutic approaches. Herein, we present a light‐activated nanocatalyst for synthesizing in situ antimicrobials through photoredox‐catalytic click reaction, achieving precise, site‐directed elimination of S. aureus skin infections. Methylene blue (MB), a commercially available photosensitizer, was encapsulated within the CuII‐based metal–organic framework, MOF‐199, and further enveloped with Pluronic F‐127 to create the light‐responsive nanocatalyst MB@PMOF. Upon exposure to red light, MB participates in a photoredox‐catalytic cycle, driven by the 1,3,5‐benzenetricarboxylic carboxylate salts (BTC) ligand presented in the structure of MOF‐199. This light‐activated MB then catalyzes the reduction of CuII to CuI through a single‐electron transfer (SET) process, efficiently initiating the click reaction to form active antimicrobial agents under physiological conditions. Both in vitro and in vivo results demonstrated the effectiveness of MB@PMOF‐catalyzed drug synthesis in inhibiting S. aureus, including their methicillin‐resistant strains, thereby accelerating skin healing in severe bacterial infections. This study introduces a novel design paradigm for controlled, on‐site drug synthesis, offering a promising alternative to realize precise treatment of bacterial infections without undesirable side effects.

Publisher

Wiley

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