Cysteamine, an Endogenous Aminothiol, and Cystamine, the Disulfide Product of Oxidation, Increase Pseudomonas aeruginosa Sensitivity to Reactive Oxygen and Nitrogen Species and Potentiate Therapeutic Antibiotics against Bacterial Infection

半胱胺是一种内源性氨基硫醇,胱胺是氧化的二硫化物产物,可增加铜绿假单胞菌对活性氧和氮物质的敏感性,并增强治疗性抗生素对抗细菌感染的能力

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作者:Douglas J Fraser-Pitt, Derry K Mercer, Daniel Smith, Aleksandra Kowalczuk, Jennifer Robertson, Emma Lovie, Peter Perenyi, Michelle Cole, Michel Doumith, Robert L R Hill, Katie L Hopkins, Neil Woodford, Deborah A O'Neil

Abstract

Cysteamine is an endogenous aminothiol produced in mammalian cells as a consequence of coenzyme A metabolism through the activity of the vanin family of pantetheinase ectoenzymes. It is known to have a biological role in oxidative stress, inflammation, and cell migration. There have been several reports demonstrating anti-infective properties targeting viruses, bacteria, and even the malarial parasite. We and others have previously described broad-spectrum antimicrobial and antibiofilm activities of cysteamine. Here, we go further to demonstrate redox-dependent mechanisms of action for the compound and how its antimicrobial effects are, at least in part, due to undermining bacterial defenses against oxidative and nitrosative challenges. We demonstrate the therapeutic potentiation of antibiotic therapy against Pseudomonas aeruginosa in mouse models of infection. We also demonstrate potentiation of many different classes of antibiotics against a selection of priority antibiotic-resistant pathogens, including colistin (often considered an antibiotic of last resort), and we discuss how this endogenous antimicrobial component of innate immunity has a role in infectious disease that is beginning to be explored and is not yet fully understood.

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