4.6 Article

Cyclic topology enhances the killing activity of polycations against planktonic and biofilm bacteria

Journal

JOURNAL OF MATERIALS CHEMISTRY B
Volume 10, Issue 25, Pages 4823-4831

Publisher

ROYAL SOC CHEMISTRY
DOI: 10.1039/d2tb00194b

Keywords

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Funding

  1. National Key R&D Program of China [2017YFA0205600, 2020YFA0710700]
  2. National Natural Science Funds for Distinguished Young Scholars [51625305]
  3. National Natural Science Foundation of China [22071232, 52073269, 81603339, 81602344, 51273187]
  4. Fundamental Research Funds for the Central Universities [YD2060002016, WK9110000005]
  5. University of Science and Technology of China [ABSL-2-2021031201]

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The study demonstrates that cyclic polycations have enhanced antibacterial activity and penetration compared to linear polycations, effectively killing both planktonic and biofilm bacteria. In a mouse infection model, cyclic polycations also show promising therapeutic effects.
Bacterial biofilms, as a fortress to protect bacteria, enhance resistance to antibiotics because of their limited penetration, which has become a major threat to current anti-infective therapy. Antimicrobial polycations have received wide attention to kill planktonic bacteria because of their unique antimicrobial mechanism without drug resistance but it is still hard to kill the bacteria in the deep of the biofilm. Unlike linear polymers, the cyclic topology has been demonstrated with enhanced penetration in tissues, which is attributed to the lack of end groups, constrained conformation and a smaller hydrodynamic volume, opening a new sight of polycations in the antibacterial application against biofilms. Here, polycations with different topologies including linear and cyclic polycations were synthesized and their killing activity against planktonic and biofilm bacteria was studied. The experimental results showed the enhanced antibacterial activity of cyclic polycations for planktonic bacteria, which is presumably attributed to their smaller hydrodynamic volume, higher local density of positive charge and more interactions between cation units and the bacterial membrane than their linear analogues. Besides, cyclic polycations exhibit enhanced killing effect for biofilm bacteria and inhibition effect for biofilms with 5-7 times and 2-3 times enhancements than the linear polycations, respectively. Furthermore, an Escherichia coli infection model on mice was established and the therapeutic effects of cyclic and linear polycations were evaluated. Compared with the linear polycations, the cyclic polycations exhibited enhanced antibacterial activity with an similar to 4 times increase, promoting the healing of the infected wounds. This work provides a new perspective in the development of antimicrobial polycations, which are promising therapeutic agents to kill planktonic and biofilm bacteria without drug resistance.

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