Literature DB >> 22430978

Pegylation of antimicrobial peptides maintains the active peptide conformation, model membrane interactions, and antimicrobial activity while improving lung tissue biocompatibility following airway delivery.

Christopher J Morris1, Konrad Beck, Marc A Fox, David Ulaeto, Graeme C Clark, Mark Gumbleton.   

Abstract

Antimicrobial peptides (AMPs) have therapeutic potential, particularly for localized infections such as those of the lung. Here we show that airway administration of a pegylated AMP minimizes lung tissue toxicity while nevertheless maintaining antimicrobial activity. CaLL, a potent synthetic AMP (KWKLFKKIFKRIVQRIKDFLR) comprising fragments of LL-37 and cecropin A peptides, was N-terminally pegylated (PEG-CaLL). PEG-CaLL derivatives retained significant antimicrobial activity (50% inhibitory concentrations [IC(50)s] 2- to 3-fold higher than those of CaLL) against bacterial lung pathogens even in the presence of lung lining fluid. Circular dichroism and fluorescence spectroscopy confirmed that conformational changes associated with the binding of CaLL to model microbial membranes were not disrupted by pegylation. Pegylation of CaLL reduced AMP-elicited cell toxicity as measured using in vitro lung epithelial primary cell cultures. Further, in a fully intact ex vivo isolated perfused rat lung (IPRL) model, airway-administered PEG-CaLL did not result in disruption of the pulmonary epithelial barrier, whereas CaLL caused an immediate loss of membrane integrity leading to pulmonary edema. All AMPs (CaLL, PEG-CaLL, LL-37, cecropin A) delivered to the lung by airway administration showed limited (<3%) pulmonary absorption in the IPRL with extensive AMP accumulation in lung tissue itself, a characteristic anticipated to be beneficial for the treatment of pulmonary infections. We conclude that pegylation may present a means of improving the lung biocompatibility of AMPs designed for the treatment of pulmonary infections.

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Year:  2012        PMID: 22430978      PMCID: PMC3370748          DOI: 10.1128/AAC.06335-11

Source DB:  PubMed          Journal:  Antimicrob Agents Chemother        ISSN: 0066-4804            Impact factor:   5.191


  45 in total

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4.  Proteolytic degradation of human antimicrobial peptide LL-37 by Bacillus anthracis may contribute to virulence.

Authors:  Joanne E Thwaite; Stephen Hibbs; Richard W Titball; Timothy P Atkins
Journal:  Antimicrob Agents Chemother       Date:  2006-07       Impact factor: 5.191

5.  A linguistic model for the rational design of antimicrobial peptides.

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Authors:  Jaleh Barar; Lee Campbell; Andrew J Hollins; Nicholas P B Thomas; Mathew W Smith; Christopher J Morris; Mark Gumbleton
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4.  Host Antimicrobial Peptides in Bacterial Homeostasis and Pathogenesis of Disease.

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5.  Novel antimicrobial peptide-modified azithromycin-loaded liposomes against methicillin-resistant Staphylococcus aureus.

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6.  Endocytic Uptake, Transport and Macromolecular Interactions of Anionic PAMAM Dendrimers within Lung Tissue.

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Review 7.  Antimicrobial peptides with selective antitumor mechanisms: prospect for anticancer applications.

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Review 8.  Molecular engineering of antimicrobial peptide (AMP)-polymer conjugates.

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9.  PEGylated Oligothioetheramide Prodrugs Activated by Host Serum Proteases.

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10.  D-BMAP18 Antimicrobial Peptide Is Active In vitro, Resists to Pulmonary Proteases but Loses Its Activity in a Murine Model of Pseudomonas aeruginosa Lung Infection.

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