Enhanced Nitric Oxide Delivery Through Self‐Assembling Nanoparticles for Eradicating Gram‐Negative Bacteria

Author:

Lai Xiangfeng1,Yu Lei2,Huang Xiangyi1,Gardner Wil3,Bamford Sarah E.3,Pigram Paul J.3,Wang Shuhong1,Brun Anton P. Le4,Muir Benjamin W.5,Song Jiangning6,Wang Yajun7,Hsu Hsien‐Yi89,Chan Philip Wai Hong2,Shen Hsin‐Hui16ORCID

Affiliation:

1. Department of Materials Science and Engineering Faculty of Engineering Monash University Clayton Victoria 3800 Australia

2. School of Chemistry Monash University Clayton VIC 3800 Australia

3. Centre for Materials and Surface Science and Department of Mathematical and Physical Sciences La Trobe University Bundoora 3086 Australia

4. Australian Centre for Neutron Scattering Australian Nuclear Science and Technology Organisation Lucas Heights NSW 2232 Australia

5. CSIRO Manufacturing Clayton VIC 3168 Australia

6. Infection and Immunity Program Monash Biomedicine Discovery Institute and Department of Microbiology Monash University Clayton VIC 3800 Australia

7. College of Chemistry & Materials Engineering Wenzhou University Shanghai Wenzhou 325027 China

8. School of Energy and Environment & Department of Materials Science and Engineering City University of Hong Kong Kowloon Tong Hong Kong

9. Shenzhen Research Institute of City University of Hong Kong Shenzhen 518057 China

Abstract

AbstractIn the current battle against antibiotic resistance, the resilience of Gram‐negative bacteria against traditional antibiotics is due not only to their protective outer membranes but also to mechanisms like efflux pumps and enzymatic degradation of drugs, underscores the urgent need for innovative antimicrobial tactics. Herein, this study presents an innovative method involving the synthesis of three furoxan derivatives engineered to self‐assemble into nitric oxide (NO) donor nanoparticles (FuNPs). These FuNPs, notably supplied together with polymyxin B (PMB), achieve markedly enhanced bactericidal efficacy against a wide spectrum of bacterial phenotypes at considerably lower NO concentrations (0.1–2.8 µg mL−1), which is at least ten times lower than the reported data for NO donors (≥200 µg mL−1). The bactericidal mechanism is elucidated using confocal, scanning, and transmission electron microscopy techniques. Neutron reflectometry confirms that FuNPs initiate membrane disruption by specifically engaging with the polysaccharides on bacterial surfaces, causing structural perturbations. Subsequently, PMB binds to lipid A on the outer membrane, enhancing permeability and resulting in a synergistic bactericidal action with FuNPs. This pioneering strategy underscores the utility of self‐assembly in NO delivery as a groundbreaking paradigm to circumvent traditional antibiotic resistance barriers, marking a significant leap forward in the development of next‐generation antimicrobial agents.

Funder

National Health and Medical Research Council

Australian Research Council

Australian Government

Publisher

Wiley

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