Analysis of the cytotoxicity of synthetic antimicrobial peptides on mouse leucocytes: implications for systemic use

doi:10.1093/jac/dkf141

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Journal of Antimicrobial Chemotherapy (2002) 50, 339-348
© 2002 The British Society for Antimicrobial Chemotherapy

Analysis of the cytotoxicity of synthetic antimicrobial peptides on mouse leucocytes: implications for systemic use

Sabrina Pacor¹^,*, Anna Giangaspero², Marina Bacac¹, Gianni Sava¹ and Alessandro Tossi²

Departments of ¹ Biomedical Sciences and ² Biochemistry, Biophysics and Macromolecular Chemistry, University of Trieste, Trieste I-34127, Italy

Received 12 February 2002; returned 5 May 2002; revised 28 May 2002; accepted 10 June 2002

We have analysed the toxicity of highly cationic, artificial ${alpha}$ -helical antimicrobial peptides on blood cells to assess theirsuitability for systemic application. Flow cytometric methods,based on the uptake of propidium iodide, were used to obtaina rapid and quantitative estimate of membrane damage to restingand concanavalin A-activated mouse lymphocytes, which was furtherconfirmed by morphological changes as observed by scanning electronmicroscopy. Membrane permeabilization appeared to correlatewith structural characteristics, so that the peptide L-19(9/B), which contains helix-stabilizing aminoisobutyricacid (Aib) residues and is a potent antimicrobial, was alsothe most lytic towards both mouse lymphocytes and human erythrocytes.Reducing the propensity for helix formation in P19(8) resultedin a marked reduction in in vitro cytotoxicity. Changing thehelical sense in D-P19(9/B) also resulted in a significant decreasein cytolytic activity towards both erythrocytes and leucocytes.A limited assessment in BALB/c mice confirmed a lower in vivotoxicity of P19(8) than L-P19(9/B). In a study of the systemicantimycotic activity of P19(8) in a mouse protection model,a modest prolongation in survival of Candida albicans-infectedanimals after intravenous administration was observed at 5 mg/kgpeptide but not at higher doses. The implications of these observationsfor the systemic use of this type of peptide are discussed.

^* Corresponding author. Tel: +39-040-5583529; Fax: +39-40-577435;E-mail: pacorsab{at}units.it

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