Membrane permeability and antimicrobial kinetics of cecropin P1 against <i>Escherichia coli</i>

Arcidiacono, Steven; Soares, Jason W.; Meehan, Alexa M.; Marek, Patrick; Kirby, Romy

doi:10.1002/psc.1125

Cited by 41 publications

(34 citation statements)

References 30 publications

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“…The region encompassing these charged residues adopts a helical confirmation. The NA-CATH structure appears to be similar to previous straight α-helical AMPs and there is strong evidence supporting a membrane disruption behavior via membrane thinning, defects, transient pores, and carpet model dissolution [20,23,32,88]. Our fluorescence and microscopy data indicate that NA-CATH functions in a similar manner.…”

Section: Resultssupporting

confidence: 70%

The structure and behavior of the NA-CATH antimicrobial peptide with liposomes

Du¹,

Samuel²,

Massiah³

et al. 2015

Biochimica et Biophysica Acta (BBA) - Biomembranes

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Naja atra cathelicidin (NA-CATH) is a 34-amino acid highly cationic peptide identified in Chinese cobras to possess potent toxicity against gram-negative and gram-positive bacteria and low toxicity against host cells. Here, we report the NMR solution structure of the full-length NA-CATH peptide and its interaction with liposomes. The structure shows a well-defined α-helix between residues Phe3 to Lys23, on which one surface is lined by the side-chains of one arginine and 11 lysine residues, while the other side is populated by hydrophobic residues. The last eleven amino acids, which are predominately aromatic and hydrophobic in nature, have no defined structure. NMR data reveal that these residues do not interact with the hydrophobic residues of the helix, indicating that the C-terminal residues have random conformations. Fluorescence requenching experiments, in which liposomes serve as a mimic of the bacterial membranes, result in fluorophore leakage that is consistent with a membrane thinning or transient pore formation mechanism. NMR titration studies of the peptide-liposome interaction reveal that the peptide is in fast exchange with the liposome, consistent with the fluorescent studies. These data indicate that full length NA-CATH possesses a helical segment and unstructured C-terminal tail that disrupts the bilayer to induce leakage and lysing.

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Section: Resultssupporting

confidence: 70%

The structure and behavior of the NA-CATH antimicrobial peptide with liposomes

Du¹,

Samuel²,

Massiah³

et al. 2015

Biochimica et Biophysica Acta (BBA) - Biomembranes

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show abstract

“…The results revealed that Mdc can mediate rapid killing of MDR- A. baumannii in 30 min and resulted in log orders of cell complete lysis at a concentration as low as 4 μ g/mL (Figure 2). These observations were in agreement with previous results obtained in other multidrug-resistant strains of bacteria with antimicrobial peptides [17]. …”

Section: Discussionsupporting

confidence: 93%

“…Many of these belong to the family of cecropin peptide [16]. Previous studies in cecropin and its related peptides demonstrate that formation of membrane-spanning pores that disrupt the cell membrane of the bacteria seems to be the most likely mechanism [17, 18]. However, the details surrounding the mechanism of bactericidal still need to be elucidated.…”

Section: Introductionmentioning

confidence: 99%

Transmission Electron Microscopic Morphological Study and Flow Cytometric Viability Assessment ofAcinetobacter baumanniiSusceptible toMusca domesticacecropin

Gui

Li²,

Feng

et al. 2014

The Scientific World Journal

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Multidrug-resistant (MDR) Acinetobacter baumannii infections are difficult to treat owing to the extremely limited armamentarium. Expectations about antimicrobial peptides' use as new powerful antibacterial agents have been raised on the basis of their unique mechanism of action. Musca domestica cecropin (Mdc), a novel antimicrobial peptide from the larvae of Housefly (Musca domestica), has potently active against Gram-positive and Gram-negative bacteria standard strain. Here we evaluated the antibacterial activity of Mdc against clinical isolates of MDR-A. baumannii and elucidate the related antibacterial mechanisms. The minimal inhibitory concentration (MIC) of Mdc was 4 μg/mL. Bactericidal kinetics of Mdc revealed rapid killing of A. baumannii (30 min). Flow cytometry using viability stain demonstrated that Mdc causes A. baumannii membrane permeabilization in a concentration- and time-dependent process, which correlates with the bactericidal action. Moreover, transmission electron microscopic (TEM) examination showed that Mdc is capable of disrupting the membrane of bacterial cells, resulting in efflux of essential cytoplasmic components. Overall, Mdc could be a promising antibacterial agent for MDR-A. baumannii infections.

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“…Figure 4 shows that dead bacteria and those treated with peptide (4x MIC) incorporated PI (63.5%), whilst bacteria without treatment did not incorporate PI. The AMP cecropin, which has been reported to induce inner membrane perturbation (Chen et al, 2003; Arcidiacono et al, 2009), induced high PI incorporation (83.75%) ( Figure 4 ).…”

Section: Resultsmentioning

confidence: 96%

“…Maximum permeability was determined by evaluating cells pre-treated with cecropin (3 μM). Permeability rate was evaluated by ONPG hydrolysis, measuring absorbance at 405 nm in 30 min intervals for up to 3 h (Arcidiacono et al, 2009). …”

Section: Methodsmentioning

confidence: 99%

A New Synthetic Peptide Having Two Target of Antibacterial Action in E. coli ML35

et al. 2016

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The increased resistance of microorganisms to the different antimicrobials available to today has highlighted the need to find new therapeutic agents, including natural and/or synthetic antimicrobial peptides (AMPs). This study has evaluated the antimicrobial activity of synthetic peptide 35409 (RYRRKKKMKKALQYIKLLKE) against Staphylococcus aureus ATCC 29213, Pseudomonas aeruginosa ATCC 15442 and Escherichia coli ML 35 (ATCC 43827). The results have shown that peptide 35409 inhibited the growth of these three bacterial strains, having 16-fold greater activity against E. coli and P. aeruginosa, but requiring less concentration regarding E. coli (22 μM). When analyzing this activity against E. coli compared to time taken, it was found that this peptide inhibited bacterial growth during the first 60 min and reduced CFU/mL 1 log after 120 min had elapsed. This AMP permeabilized the E. coli membrane by interaction with membrane phospholipids, mainly phosphatidylethanolamine, inhibited cell division and induced filamentation, suggesting two different targets of action within a bacterial cell. Cytotoxicity studies revealed that peptide 35409 had low hemolytic activity and was not cytotoxic for two human cell lines. We would thus propose, in the light of these findings, that the peptide 35409 sequence should provide a promising template for designing broad-spectrum AMPs.

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Membrane permeability and antimicrobial kinetics of cecropin P1 against Escherichia coli

Cited by 41 publications

References 30 publications

The structure and behavior of the NA-CATH antimicrobial peptide with liposomes

The structure and behavior of the NA-CATH antimicrobial peptide with liposomes

Transmission Electron Microscopic Morphological Study and Flow Cytometric Viability Assessment ofAcinetobacter baumanniiSusceptible toMusca domesticacecropin

A New Synthetic Peptide Having Two Target of Antibacterial Action in E. coli ML35

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