Multi-targets of antimicrobial photodynamic therapy mediated by erythrosine against Staphylococcus aureus identified by proteomic approach

Staphylococcus aureus is a global challenge to the clinical field and food industry. Therefore, the development of antimicrobial photodynamic therapy (aPDT) has become one of the valuable methods to control this pathogen. The antibacterial activity of photoinactivation by erythrosine (Ery) against S...

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Veröffentlicht in:Photochemistry and photobiology 2024-11, Vol.100 (6), p.1848-1863
Hauptverfasser: de Oliveira Silva, João Vitor, Meneguello, Jean Eduardo, Formagio, Maíra Dante, de Freitas, Camila Fabiano, Malacarne, Luis Carlos, Marchiosi, Rogério, de Mendonça, Patrícia de Souza Bonfim, Zanetti Campanerut-Sá, Paula Aline, Graton Mikcha, Jane Martha
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Sprache:eng
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Zusammenfassung:Staphylococcus aureus is a global challenge to the clinical field and food industry. Therefore, the development of antimicrobial photodynamic therapy (aPDT) has become one of the valuable methods to control this pathogen. The antibacterial activity of photoinactivation by erythrosine (Ery) against S. aureus has been reported, but its modes of action are unclear. This study aimed to employ a proteomic approach to analyze modes of action of Ery-aPDT against S. aureus. We determined the antibacterial effect by Ery-aPDT assays, quantified reactive oxygen species (ROS) and injury to the cell membrane, and determined protein expression using a proteomic approach combined with bioinformatic tools. Ery-aPDT was effective in reducing S. aureus to undetectable levels. In addition, the increment of ROS accompanied the increase in the reduction of cell viability, and damage to cellular membranes was shown by sublethal injury. In proteomic analysis, we found 17 differentially expressed proteins. These proteins revealed changes mainly associated with defense to oxidative stress, energy metabolism, translation, and protein biosynthesis. Thus, these results suggest that the effectiveness of Ery-aPDT is due to multi-targets in the bacterial cell that cause the death of S. aureus.
ISSN:0031-8655
1751-1097
1751-1097
DOI:10.1111/php.13944