4.6 Article

Bacterial-Specific Aggregation and Killing of Immunomodulatory Host Defense Peptides

Journal

PHARMACEUTICALS
Volume 14, Issue 9, Pages -

Publisher

MDPI
DOI: 10.3390/ph14090839

Keywords

antibacterial peptides; bacterial flocculation; nonhemolytic; immunomodulatory

Funding

  1. Natural Sciences and Engineering Research Council Discovery Grant (NSERC-DG) [RGPIN-06183/2018]
  2. Canadian Poultry Research Council (CPRC)

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This study focuses on the design and development of disulfide bridge-linked antimicrobial peptides using Angiogenin 4 (chAng4) as a template. The results demonstrate that the synthetic mCA4 peptides show superior antibacterial efficacies, are non-toxic and non-hemolytic, and can mediate bacterial flocculation and killing without external stimuli.
This study involves the design and development of disulfide bridge-linked antimicrobial peptides using the host defense protein Angiogenin 4 (chAng4) as a template. The mini peptides derived from chAng4 (mCA4s) were evaluated for their antibacterial efficacies in various pathogenic bacterial strains, and the role of the oxidation state of thiols in the peptide sequence and its implication on antibacterial properties were explored. A remarkable property of these synthetic mCA4 peptides is their capability to flocculate bacteria and mediate bacterial-specific killing, in the absence of any other external stimulus. mCA4s were further evaluated for their cellular uptake, hemolytic activities, toxicities, and immunomodulatory activities in different eukaryotic cell lines. The results indicate that disulfide bridge-containing cationic amphipathic peptides show superior antibacterial efficacies, are nontoxic and nonhemolytic, and mediate bacterial flocculation and killing, in the absence of external stimuli.

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