A CcdB toxin-derived peptide acts as a broad-spectrum antibacterial therapeutic in infected mice.
Jayantika BhowmickManish NagPritha GhoshRaju S RajmaniRitika ChatterjeeKapudeep KarmakarKasturi ChandraJayanta ChatterjeeDipshikha ChakravorttyRaghavan VaradarajanPublished in: EMBO reports (2023)
The bacterial toxin CcdB (Controller of Cell death or division B) targets DNA Gyrase, an essential bacterial topoisomerase, which is also the molecular target for fluoroquinolones. Here, we present a short cell-penetrating 24-mer peptide, CP1-WT, derived from the Gyrase-binding region of CcdB and examine its effect on growth of Escherichia coli, Salmonella Typhimurium, Staphylococcus aureus and a carbapenem- and tigecycline-resistant strain of Acinetobacter baumannii in both axenic cultures and mouse models of infection. The CP1-WT peptide shows significant improvement over ciprofloxacin in terms of its in vivo therapeutic efficacy in treating established infections of S. Typhimurium, S. aureus and A. baumannii. The molecular mechanism likely involves inhibition of Gyrase or Topoisomerase IV, depending on the strain used. The study validates the CcdB binding site on bacterial DNA Gyrase as a viable and alternative target to the fluoroquinolone binding site.
Keyphrases
- acinetobacter baumannii
- escherichia coli
- pseudomonas aeruginosa
- multidrug resistant
- drug resistant
- klebsiella pneumoniae
- staphylococcus aureus
- cell death
- biofilm formation
- circulating tumor
- single molecule
- listeria monocytogenes
- cell free
- gram negative
- cystic fibrosis
- bone marrow
- nucleic acid
- cell therapy
- metabolic syndrome
- stem cells
- transcription factor
- high fat diet induced
- insulin resistance