AI Article Synopsis

  • The study highlights the declining effectiveness of traditional antibiotics against MRSA and suggests combining natural products, like theaflavin (TF), with existing antibiotics as a new treatment strategy.
  • Molecular docking results reveal that TF binds to the allosteric site of PBP2a, which helps open the active site for better interaction with β-lactam antibiotics, potentially enhancing their effectiveness against MRSA.
  • Experimental tests confirm that the combination of TF and ceftiofur shows improved antibacterial effects compared to either treatment alone, and this synergy was also observed in a mouse model of MRSA-induced pneumonia.

Article Abstract

Recurrent epidemics of methicillin-resistant () (MRSA) have illustrated that the effectiveness of antibiotics in clinical application is rapidly fading. A feasible approach is to combine natural products with existing antibiotics to achieve an antibacterial effect. In this molecular docking study, we found that theaflavin (TF) preferentially binds the allosteric site of penicillin-binding protein 2a (PBP2a), inducing the PBP2a active site to open, which is convenient for β-lactam antibiotics to treat MRSA infection, instead of directly exerting antibacterial activity at the active site. Subsequent TMT-labeled proteomics analysis showed that TF treatment did not significantly change the landscape of the USA300 proteome. Checkerboard dilution tests and kill curve assays were performed to validate the synergistic effect of TF and ceftiofur, and the fractional inhibitory concentration index (FICI) was 0.1875. The antibacterial effect of TF combined with ceftiofur was better than that of single-drug treatment . In addition, TF effectively enhanced the activity of ceftiofur in a mouse model of MRSA-induced pneumonia. Our findings provide a potential therapeutic strategy to combine existing antibiotics with natural products to resolve the prevalent infections of multidrug-resistant pathogens.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9702817PMC
http://dx.doi.org/10.3389/fmicb.2022.993430DOI Listing

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