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Please use this identifier to cite or link to this item: https://hdl.handle.net/2440/4440
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Type: Journal article
Title: Maculatin 1.1, an anti-microbial peptide from the Australian tree frog, Litoria genimaculata: Solution structure and biological activity
Author: Chia, C.
Carver, J.
Mulhern, T.
Bowie, J.
Citation: The Federation of European Biochemical Societies (FEBS) Journal, 2000; 267(7):1894-1908
Publisher: Blackwell Science Ltd
Issue Date: 2000
ISSN: 1742-464X
0014-2956
Statement of
Responsibility: 		Brian C. S. Chia, John A. Carver, Terrence D. Mulhern and John H. Bowie
Abstract: The dorsal glands of Australian tree frogs from the Litoria species contain a diversity of antibiotic peptides that forms part of the defence system of the animal. Here, the antibiotic activity and structure of maculatin 1.1, a 21 amino acid peptide from Litoria genimaculata, are compared. The activity data on maculatin 1.1 and a series of its analogues imply that the mechanism of action of maculatin 1.1 involves binding to, and subsequent lysis of, the bacterial cell membrane. The structure of maculatin 1.1 was determined using NMR spectroscopy in a trifluoroethanol/water mixture and when incorporated into dodecylphosphocholine micelles. Under both conditions, the peptide adopts a very similar conformation, i.e. a helical structure with a central kink in the vicinity of Pro15. The kink allows the peptide to adopt a well-defined amphipathic conformation along its entire length. The similar structures determined under both solvent conditions imply that structures of membraneinteracting peptides in trifluoroethanol/water mixtures are representative of those adopted in a membrane environment, e.g. when incorporated into micelles. The synthetic Ala15 analogue of maculatin 1.1 has markedly reduced activity and its NMR-derived structure is a well-defined helix, which lacks the central kink and flexibility of the parent molecule. It is concluded that the kink is important for full biological activity of the peptide, probably because it allows maximum amphipathicity of the peptide to facilitate interaction with the membrane. The structure of maculatin 1.1 is compared with a related peptide, caerin 1.1 [Wong, H., Bowie, J.H. and Carver, J.A. (1997) Eur. J. Biochem. 247, 545±557], which has an additional central proline residue and enhanced central flexibility compared with maculatin 1.1. The role of central flexibility within antibiotic peptides in their interaction with bacterial membranes is discussed.
Keywords: amphipathic helix
anti-microbial peptide
NMR spectroscopy
solution structure
Description: Published in European Journal of Biochemistry, 2000; 267 (7):1894-1908 at www.interscience.wiley.com Copyright © 2000 FEBS
Provenance: Titled FEBS Journal from 2005 and published by Wiley from 2008.
Published Online: 25 Dec 2001
DOI: 10.1046/j.1432-1327.2000.01089
Published version: http://www3.interscience.wiley.com/cgi-bin/fulltext/119181854/PDFSTART
Appears in Collections:Aurora harvest 2
Chemistry publications

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