The anti-platelet drug ticlopidine inhibits FapC fibrillation and biofilm production: Highlighting its antibiotic activity

The anti-platelet drug ticlopidine inhibits FapC fibrillation and biofilm production: Highlighting its antibiotic activity

Multidrug resistance of bacteria and persistent infections related to biofilms, as well as the low availability of new antibacterial drugs, make it urgent to develop new antibiotics. Here, we evaluate the antibacterial and anti-biofilm properties of ticlopidine (TP), an anti-platelet aggregation dru...

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Veröffentlicht in:Biochimica et biophysica acta. Proteins and proteomics 2023-02, Vol.1871 (2), p.140883-140883, Article 140883
Hauptverfasser: Pirhaghi, Mitra, Najarzadeh, Zahra, Moosavi-Movahedi, Faezeh, Shafizadeh, Mahshid, Mamashli, Fatemeh, Atarod, Deyhim, Ghasemi, Atiyeh, Morshedi, Dina, Meratan, Ali Akbar, Otzen, Daniel E., Saboury, Ali Akbar
Format: Artikel
Sprache:eng
Schlagworte:
Amyloid fibrillation
Anti-Bacterial Agents - chemistry
Anti-Bacterial Agents - pharmacology
Antibacterial
Bacterial biofilm
Biofilms
Escherichia coli
FapC
Gram-Negative Bacteria - physiology
Gram-Positive Bacteria
Humans
Ticlopidine
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Zusammenfassung:Multidrug resistance of bacteria and persistent infections related to biofilms, as well as the low availability of new antibacterial drugs, make it urgent to develop new antibiotics. Here, we evaluate the antibacterial and anti-biofilm properties of ticlopidine (TP), an anti-platelet aggregation drug, TP showed antibacterial activity against both gram-positive (MRSA) and gram-negative (E. coli, and P. aeruginosa) bacteria over a long treatment period. TP significantly reduced the survival of gram-negative bacteria in human blood though impact on gram-positives was more limited. TP may cause death in MRSA by inhibiting staphyloxanthin pigment synthesis, leading to oxidative stress, while scanning electron microscopy imaging indicate a loss of membrane integrity, damage, and consequent death due to lysis in gram-negative bacteria. TP showed good anti-biofilm activity against P. aeruginosa and MRSA, and a stronger biofilm degradation activity on P. aeruginosa compared to MRSA. Measuring fluorescence of the amyloid-reporter Thioflavin T (ThT) in biofilm implicated inhibition of amyloid formation as part of TP activity. This was confirmed by assays on the purified protein in P. aeruginosa, FapC, whose fibrillation kinetics was inhibited by TP. TP prolonged the lag phase of aggregation and reduced the subsequent growth rate and prolonging the lag phase to very long times provides ample opportunity to exert TP's antibacterial effect. We conclude that TP shows activity as an antibiotic against both gram-positive and gram-negative bacteria thanks to a broad range of activities, targeting bacterial metabolic processes, cellular structures and the biofilm matrix. [Display omitted] •Long treatment period antibacterial activity of Ticlopidine against Gram-positive and Gram-negative bacteria•Anti-biofilm and biofilm degradation activity of Ticlopidine•Inhibition of biofilm amyloid formation as part of Ticlopidine activity•Broad range of activities of Ticlopidine, targeting bacterial metabolic processes, cellular structures and the biofilm matrix
ISSN:1570-9639
1878-1454
DOI:10.1016/j.bbapap.2022.140883