Inflammatory Microenvironment‐Responsive Hydrogels Enclosed with Quorum Sensing Inhibitor for Treating Post‐Traumatic Osteomyelitis

Author:

Zhang Wenting123,Lu Huidan123,Zhang Wanying123,Hu Jiahao4,Zeng Yifei123,Hu Huiqun123,Shi Liyun5,Xia Jingyan6,Xu Feng123ORCID

Affiliation:

1. Department of Infectious Diseases The Second Affiliated Hospital Zhejiang University School of Medicine Hangzhou Zhejiang 310009 China

2. Key Laboratory of Multiple Organ Failure (Zhejiang University), Ministry of Education Hangzhou 310053 China

3. Research Center for Life Science and Human Health Binjiang Institute of Zhejiang University Hangzhou 310053 China

4. Department of General Surgery Sir Run‐Run Shaw Hospital Zhejiang University School of Medicine Hangzhou Zhejiang 310016 China

5. Institute of Translational Medicine Zhejiang Shuren University Hangzhou Zhejiang 310015 China

6. Department of Radiation Therapy The Second Affiliated Hospital Zhejiang University School of Medicine Hangzhou Zhejiang 310009 China

Abstract

AbstractNon‐antibiotic strategies are desperately needed to treat post‐traumatic osteomyelitis (PTO) due to the emergence of superbugs, complex inflammatory microenvironments, and greatly enriched biofilms. Previously, growing evidence indicated that quorum sensing (QS), a chemical communication signal among bacterial cells, can accelerate resistance under evolutionary pressure. This study aims to develop a medical dressing to treat PTO by inhibiting QS and regulating the inflammatory microenvironment, which includes severe oxidative stress and acid abscesses, through a reactive oxygen species (ROS)‐responsive bond between N1‐ (4‐borobenzoyl)‐N3‐(4‐borobenzoyl)‐the N1, the N1, N3, N3‐tetramethylpropane‐1,3‐diamine (TSPBA) and polyvinyl alcohol (PVA), and the amino side chain of hyperbranched polylysine (HBPL). Physically enclosed QS inhibitors subsequently exerted the antibacterial effects. This hydrogel can scavenge hydrogen peroxide (H2O2), superoxide anion free radical (·O2), hydroxyl radicals (·OH) and 2,2‐di(4‐tert‐octylphenyl)‐1‐picryl‐hydrazyl (DPPH) to reduce oxidative stress and inhibit “bacteria‐to‐bacteria communication”, thus clearing planktonic bacteria and biofilms, accelerating bacterial plasmolysis, reducing bacterial virulence and interfering with membrane transport. After in vivo treatment with hydrogel, nearly all bacteria are eliminated, inflammation is effectively inhibited, and osteogenesis and bone repair are promoted to facilitate recovery from PTO. The work demonstrates the clinical translational potential of the hydrogel in the treatment of drug‐resistant bacteria induced PTO.

Funder

National Natural Science Foundation of China

Publisher

Wiley

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