4.8 Article

Environmentally sensitive photosensitizers enable targeted photodynamic ablation of Gram-positive antibiotic resistant bacteria

期刊

THERANOSTICS
卷 13, 期 11, 页码 3814-3825

出版社

IVYSPRING INT PUBL
DOI: 10.7150/thno.84187

关键词

photodynamic therapy; antimicrobial resistance; probes; biofilms; theranostic agents

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Bacterial infections pose significant challenges to human health, leading to high antibiotic usage, morbidity, hospitalizations, and approximately 8 million deaths worldwide annually. The overuse of antibiotics and lack of antimicrobial innovations have resulted in antimicrobial resistant pathogens that may reverse the progress of modern medicine. Photodynamic therapeutics have the potential to kill bacteria, but there are limited agents that can target pathogens effectively with minimal off-target effects.
Bacterial infections remain among the biggest challenges to human health, leading to high antibiotic usage, morbidity, hospitalizations, and accounting for approximately 8 million deaths worldwide every year. The overuse of antibiotics and paucity of antimicrobial innovation has led to t antimicrobial resistant pathogens that threaten to reverse key advances of modern medicine. Photodynamic therapeutics can kill bacteria but there are few agents that can ablate pathogens with minimal off-target effects. Methods: We describe nitrobenzoselenadiazoles as some of the first environmentally sensitive organic photosensitizers, and their adaptation to produce theranostics with optical detection and light-controlled antimicrobial activity. We combined nitrobenzoselenadiazoles with bacteria-targeting moieties (i.e., glucose-6-phosphate, amoxicillin, vancomycin) producing environmentally sensitive photodynamic agents.Results: The labelled vancomycin conjugate was able to both visualize and eradicate multidrug resistant Gram-positive ESKAPE pathogens at nanomolar concentrations, including clinical isolates and those that form biofilms.Conclusion: Nitrobenzoselenadiazole conjugates are easily synthesized and display strong environment dependent ROS production. Due to their small size and non-invasive character, they unobtrusively label antimicrobial targeting moieties. We envisage that the simplicity and modularity of this chemical strategy will accelerate the rational design of new antimicrobial therapies for refractory bacterial infections.

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